Gynaecology Flashcards

1
Q

Common presenting complaints in gynecology?

A

▪ Heavy/painful/irregular or absent periods
▪ Pelvic pain/pain on intercourse
▪ Urinary incontinence
▪ ‘something coming down’ (prolapse)
▪ Infertility
▪ Request for sterilisation
▪ Bleeding or pain in early pregnancy
▪ Postmenopausal bleeding
▪ Vaginal discharge

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2
Q

What should be asked about in a menstrual history?

A

First and last day of last menstrual period (LMP)

Any abnormal bleeding: intermenstrual or post coital bleeding

Menarche (age at first period)

Frequency – average 28 days <24 days Frequent, >38 days Infrequent
Duration of bleeding – average 5 days (>8 days Prolonged, <4.5 days shortened)

Volume – average 40ml menstrual blood loss over course of menses
>80ml heavy (Hb and Ferritin affected), <5ml Light
Women may describe ‘flooding’ and clots passed

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3
Q

What might you ask a patient about contraception when history taking?

A

Current method and duration of use
Previous methods - what method, length of use, why it was stopped, when it was stopped
Any problems with contraception
Hx of migraines with aura if considering COCP

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4
Q

What might you ask a patient about cervical smears when taking a gynae history?

A

When a smear was last taken
What was the result

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5
Q

What might be relevant to obstetric history?

A

Gravidity (number of pregnancies)
Parity (number of births of gestation last 24 weeks)
Pregnancy outcomes
Birth weights
Modes of delivery - vaginal, assisted vaginal (forceps), c section
When births occurred (at term)
Prv baby weight
Any miscarriages - when - medical, spontaneous, surgical (D&C)
Antenatal checks - chromosomal abnormalities testing?? Bloods, 11-14 week dating scan, 20 week abnormality scan

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6
Q

What might be relevant in a past gynaecology history?

A

Past gynaecological problems, their investigations and treatment
Previous gynaecological operations
Past genitourinary infections
Smears
Contraception
Menstural history
Sexual history including STIs

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7
Q

Basic structure of gynaecological history?

A

Demographic and reproductive identifiers

Presenting complaint (elaborate, impact on QOL and normal functioning)

Menstrual history

Contraception

Sexual history

Possibility of pregnancy

Cervical smear

Obstetric history and plans for future pregnancies

Previous gynaecological history

Past medical history

DHx inc allergies

Social hx including smoking and alcohol

FHx

System inquires

ICE

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8
Q

Describe the mechanism of action in tranexamic acid in the management of heavy menstrual blood loss

A

Fibrinolytic drug

TXA is a synthetic reversible competitive inhibitor to the lysine receptor found on plasminogen. The binding of this receptor prevents plasmin (activated form of plasminogen) from binding to and ultimately stabilizing the fibrin matrix and therefore bleeding.

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9
Q

Describe the mechanism of action in mefanamic acid in the management of heavy menstrual blood loss and dysmenorrhea?

A

NSAID, works by inhibition of prostaglandin synthesis + reduces the activity of prostaglandins in the uterus lining which are elevated in women with heavy bleeding.
Prostaglandins are hormones which cause pain and inflammation

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10
Q

What is hematometra and why might it occur?

A

Hematometra is a collection or retention of blood in the uterus most commonly due to an imperforate hymen or transverse vaginal septum.

Acquired causes leading to cervical stenosis include radiation treatment, ablation, cervical conization, or malignancies

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11
Q

Causes of menorrhagia?

A

Dysfunctional uterine bleeding (no identifiable cause)
Extremes of reproductive age
Fibroids
Endometriosis and adenomyosis
Pelvic inflammatory disease (infection)
Contraceptives, particularly the copper coil
Anticoagulant medications
Bleeding disorders (e.g. Von Willebrand disease)
Endocrine disorders (diabetes and hypothyroidism)
Connective tissue disorders
Endometrial hyperplasia or cancer
Polycystic ovarian syndrome

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12
Q

The PALM-COEIN system divides the causes into structural (‘PALM’) and non-structural (‘COEIN’) - what are the structural causes of menorrhagia?

A

Polyps
Adenomyosis
Leiomyoma (fibroid)
Malignancy of endometrial hypoplasia (this includes bleeding from vaginal or cervical malignancies, or that provoked by ovarian tumours)

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13
Q

The PALM-COEIN system divides the causes into structural (‘PALM’) and non-structural (‘COEIN’) - what are the non-structural causes of menorrhagia?

A

Coagulopathy (Von Willebrand’s disease is the most common coagulopathy to cause heavy menstrual bleeding, also consider warfarin therapy)
Ovarian dysfunction (PCOS, hypothyroidism)
Endometriosis
Iatrogenic (E.g. contraceptive hormones, copper IUD.)
No identifiable cause (DUB)

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14
Q

What features might suggest an underlying coagulopathy in a patient presenting with HMB (menorrhagia)

A

HMB since menarche
History of post-partum haemorrhage
Surgical related bleeding or dental related bleeding; Easy bruising/epistaxis
Bleeding gums
Family history of bleeding disorder

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15
Q

How might fibroids present?

A

Bulky uterus O/E
HMB
Hx of pressure symptoms (urinary freq, constipation)

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16
Q

What volume of blood loss during a period would affects Hb and Ferritin?

A

> 80ml
Anaemia from 120ml

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17
Q

Most patients presenting with menorrhagia (heavy menstrual bleeding) should be examined (pelvic examination with speculum and bimanual) - what should be looked out for?

A

Pallor (anaemia)
Palpable uterus or pelvic mass
Try to ascertain if the uterus is smooth or irregular (fibroids)
A tender uterus or cervical excitation point toward adenomyosis/endometriosis
Inflamed cervix/cervical polyp/cervical tumour
Vaginal tumour
Ascities

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18
Q

Main features of HMB (menorrhagia)

A

Bleeding during menstruation deemed to be excessive for the individual woman (>80ml): changing pads every 1-2 hours, bleeding lasting more than 7 days or passing very large clots.
Fatigue.
Shortness of breath (if associated anaemia).

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19
Q

Main risk factors for heavy menstrual bleeding (menorrhagia)?

A

The two main risk factors for heavy menstrual bleeding are age (more likely at menarche and approaching the menopause), and obesity.

There are also other risk factors that relate to the specific causes of HMB. One example would be previous caesarean section – as a risk factor for adenomyosis.

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20
Q

What is HMB?

A

Heavy menstrual bleeding - excessive menstrual loss, bleeding not related to pregnancy and occurring only within the woman’s reproductive years (ie. not post-menopausal bleeding).

Diagnosis based on symptoms - such as changing pads every 1-2 hours, bleeding lasting more than 7 days, passing large blood clots.

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21
Q

Most patients presenting with menorrhagia (heavy menstrual bleeding) should be examined (pelvic examination with speculum and bimanual) - when might they not require PV examination?

A

Straightforward hx HMB without other risk factors or symptoms

Patients who are young and not sexually active

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22
Q

What investigation should be performed in all women with HMB and why?

A

Full blood count - to look for iron deficiency anaemia

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23
Q

What bloods might be performed in a women presenting with HMB?

A

Full blood count:
Anaemia tends to present after menstrual blood loss of 120ml.

Thyroid function test:
If other signs and symptoms of underactive thyroid.

Other hormone testing:
Not routine but considered if other clinical features e.g. suspicion of Polycystic ovary syndrome.

Coagulation screen + test for Von Willebrand’s:
If suspicion of clotting disorder on history taking.

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24
Q

HMB: imaging, histology and microbiology

A

Ultrasound pelvis
Transvaginal US is most clinically useful for assessing the endometrium and ovaries.
It should be considered if the uterus or a pelvic mass is palpable on examination, or if pharmacological treatment has failed.

Cervical smear
No need to repeat if up to date.

High vaginal and endocervical swabs for infection.

Pipelle endometrial biopsy:
(if persistent intermenstrual bleeding, >45 years old, and/or failure of pharmacological treatment.)

Hysteroscopy and endometrial biopsy:
(Typically performed when ultrasound identifies pathology, or is inconclusive)

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25
Q

Indications for pipelle endometrial biopsy in a patient presenting with HMB?

A

Persistent IMB, >45 years old, and/or failure of pharmacological treament

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26
Q

When should outpatient hysteroscopy be arranged in a patient presenting with HMB?

A

Suspected submucosal fibroids

Suspected endometrial pathology, such as endometrial hyperplasia or cancer

Persistent intermenstrual bleeding

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27
Q

When should pelvic and transvaginal ultrasound be arranged in a patient presenting with HMB?

A

Possible large fibroids (palpable pelvic mass)

Possible adenomyosis (associated pelvic pain or tenderness on examination)

Examination is difficult to interpret (e.g. obesity)

Hysteroscopy is declined

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28
Q

Medical management of HMB?

A

Management of identifiable cause

Symptomatic relief (non contraceptive): tranexamic acid or mefenamic acid

Contraception: Minera coil (1st line), COCP, cyclical oral progestogens, progesterone only contraception (depo, implant POP)
NB: oral norethisterone (Taken day 5-26 of cycle) does not work as a contraceptive when taken in this manner

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29
Q

Management of HMB where medical management has failed?

A

Endometrial ablation

Hysterectomy (subtotal or total, ovaries not removed unless abnormal. Can be performed through abdominal incision or through the vagina

Fibroids: myomectomy and uterine artery embolism

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30
Q

When is referral to secondary care for further investigation and management indicated for patients with HMB?

A

Referral to secondary care for further investigation and management is indicated if treatment is unsuccessful, symptoms are severe or there are large fibroids (more than 3 cm).

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31
Q

Levonorgestral-releasing intrauterine system (LNG-IUS) - use in HMB

A

First line contraceptive option

Also acts as a contraceptive.
Is licensed for 5 years treatment.
Thins endometrium and can shrink fibroids.

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32
Q

When is oral norethisterone taken when used to manage HMB

A

(Taken day 5-26 of cycle)

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33
Q

Tranexamic acid, mefanamic acid - advantages in treating HMB?

A

No effect on fertility
Non-hormonal
Mefenamic acid also analgesic

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34
Q

What is a hysterectomy?

A

A hysterectomy is the surgical removal of the uterus. It is a very common procedure, performed for a variety of indications.

It can be classified by the amount of tissue resected

Total hysterectomy
Sub-total hysterectomy
Total hysterectomy and bilateral salpingo-oophorectomy
Radical hysterectomy

There are three main approaches to a hysterectomy. The principles and steps for each approach are the same (but in a different order).

Abdominal – via an incision in the abdomen.
Vaginal – via incision through the superior part of the vagina.
Laparoscopic – via small incisions in the abdomen, and using laparoscopes and a uterine manipulator.

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35
Q

What is a total hysterectomy?

A

removal of the uterus and cervix

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36
Q

What is a sub-total hysterectomy

A

removal of the body of the uterus only (leaving the cervix behind)

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37
Q

What is a total hysterectomy and bilateral salpingo-oophorectomy?

A

removal of the uterus, cervix, fallopian tubes and ovaries.

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38
Q

What is a radical hysterectomy and why might it be performed?

A

Removal of:
Uterus
Cervix
Parametrium
Vaginal cuff
Part of or entire fallopian tubes
Ovaries may be removed or left behind (depending on the patients age)

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39
Q

Mobilization + discharge - hysterectomy?

A

Mobilisation should be encouraged as soon as possible.

Discharge is usually after 1-2 days for vaginal and laparoscopic hysterectomy, and 2-5 days for abdominal hysterectomy (depending on the type of incision – generally longer stay if midline incision).

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40
Q

What incision is used to perform and abdominal hysterectomy?

A

Depends on uterus size and indication

Low transverse incision

Midline incision (may be necessitated in a large fibroid uterus for example)

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41
Q

What type of anesthetic is used in a hysterectomy?

A

Abdominal and laproscopic hysterectomy are perfomed under general anestethic

Vaginal hysterectomy may be performed under regional anaesthesia (spinal/ epidural). A general anaesthetic is not required.

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42
Q

Indications for hysterectomy?

A

Heavy menstrual bleeding

Pelvic pain

Uterine prolapse (vaginal hysterectomy
)
Gynaecological malignancy (usually ovarian, uterine or cervical)

Risk reducing surgery, usually in cases of BRCA 1 or 2 mutations, or Lynch syndrome.

Hysterectomy may also be performed as a life saving procedure in the management of major postpartum haemorrhage.

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43
Q

There are some potential complications of a hysterectomy. As for any surgical procedure, the general complications include risk of haemorrhage, infection and pain. There is also a general anaesthetic risk. What do the procedure specific complications include?

A

Damage to bladder and/or uterter and/or long term distrbance to bladder function

Damage to the bowel

Hemorrhage requiring blood tranfusion (relatively common)

Return to theatre: bleeding/wound dehissince

Pelvic abscess/infection

VTE or PE

Risk of death within 6 weeks, 32 women in every 100 000 (rare). The main causes of death are pulmonary embolism and cardiac disease.

If the ovaries are conserved, menopause may occur earlier (by 1-2 years) due to a change in the blood supply to the ovaries.

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44
Q

What is dysmenorrhea?

A

Dysmenorrhoea or “painful periods” is the most common of all gynaecological symptoms. It is generally described as a crampy lower abdominal pain, which starts at the onset of menstruation.

It can be classified as either:

Primary – menstrual pain occurring with no underlying pelvic pathology.
Secondary – menstrual pain that occurs with an associated pelvic pathology.

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45
Q

Aetiology and pathophysiology of dysmenorrhea

A

In the absence of fertilisation of the egg, the corpus luteum regresses, and there is a subsequent decline in oestrogen and progesterone production.

The endometrial cells are sensitive to this decline in progesterone, and respond with prostaglandin release. Prostaglandins have two main actions in the uterus:

Spiral artery vasospasm – leading to ischaemic necrosis and shedding of the superficial layer of the endometrium.

Increased myometrial contractions.

Primary dysmenorrhoea is thought to occur secondary to the excessive release of prostaglandins (PGF2α and PGE2) by endometrial cells.

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46
Q

What are the risk factors for primary dysmenorrhoea?

A

Early menarche
Long menstrual phase
Heavy periods
Smoking
Nuliparity

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47
Q

Clinical features of dysmenorrhoea?

A

The typical description of dysmenorrhoea is lower abdominal or pelvic pain, which can radiate to lower back or anterior thigh.

Pain is crampy in nature. It usually lasts for 48-72 hours around the menstrual period, and is characteristically worst at the onset of menses.

The pain can be associated with other symptoms, such as; malaise, nausea, vomiting, diarrhoea, dizziness.

Abdominal and pelvic examinations (including speculum examination of cervix) are performed but are usually unremarkable. Uterine tenderness may be present.

Note: Dysmenorrhoea may resolve following pregnancy.

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48
Q

Causes of secondary dysmenorrhoea?

A

Endometriosis
Adenomyosis
Pelvic inflammatory disease
Adhesions

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49
Q

Dysmenorrhoea - investigations?

A

No investigations are specific to primary dysmenorrhoea and therefore the work up is focused on ruling out underlying pathology.

If the patient is at high risk of a sexually transmitted infection, then a high vaginal swab and endocervical swabs are indicated to screen for underlying infection.

If on examination a pelvic mass is palpated, a transvaginal ultrasound scan (TVS) should be performed to investigate further.

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50
Q

Management of dysmenorrhoea?

A

Lifestyle Changes:

Stop smoking (there is a clear relationship between smoking and dysmenorrhoea).

Pharmacological:

Anagelsia (First line):
NSAIDs (ibuprofen, naproxen, mefenamic acid). They work by inhibiting the production of prostaglandins; which have been implicated in the pathogenesis of primary dysmenorrhoea.
And/or paracetamol
3-6 month trial of hormonal contraception (Second line):
Monophasic combined oral contraceptive pill is most commonly used first line.
Intrauterine system (e.g Mirena coil) may also be effective.

Non-Pharmacological

Local application of heat (water bottles or heat patch)

Transcutaneous Electrical Nerve Stimulation (TENS)

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51
Q

What is amenorrhoea?

A

Amenorrhoea refers to a lack of menstrual periods.

Primary amenorrhoea is when the patient has never developed periods.

Secondary amenorrhoea is when the patient previously had periods that subsequently stopped.

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52
Q

What is abnormal uterine bleeding and why might it occur?

A

Abnormal uterine bleeding refers to irregularities in the menstrual cycle, affecting frequency, duration, regularity of the cycle length and the volume of menses. Irregular menstrual periods indicate anovulation (a lack of ovulation) or irregular ovulation. This occurs due to disruption of the normal hormonal levels in the menstrual cycle, or ovarian pathology. It can be due to:

Extremes of reproductive age (early periods or perimenopause)
Polycystic ovarian syndrome
Physiological stress (excessive exercise, low body weight, chronic disease and psychosocial factors)
Medications, particularly progesterone only contraception, antidepressants and antipsychotics
Hormonal imbalances, such as thyroid abnormalities, Cushing’s syndrome and high prolactin

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53
Q

What is IMB?

A

Intermenstrual bleeding (IMB) refers to any bleeding that occurs between menstrual periods. This is a red flag that should make you consider cervical and other cancers, although other causes are more common.

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54
Q

What are the key causes of IMB?

A

Hormonal contraception
Cervical ectropion, polyps or cancer
Sexually transmitted infection
Endometrial polyps or cancer
Vaginal pathology, including cancers
Pregnancy
Ovulation can cause spotting in some women
Medications, such as SSRIs and anticoagulants

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55
Q

What is dysmenorrhea and why might it occur?

A

Dysmenorrhoea describes painful periods. The causes are:

Primary dysmenorrhoea (no underlying pathology)
Endometriosis or adenomyosis
Fibroids
Pelvic inflammatory disease
Copper coil
Cervical or ovarian cancer

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56
Q

What is menorrhagia and why might it occur?

A

Menorrhagia refers to heavy menstrual bleeding. This can be caused by:

Dysfunctional uterine bleeding (no identifiable cause)
Extremes of reproductive age
Fibroids
Endometriosis and adenomyosis
Pelvic inflammatory disease (infection)
Contraceptives, particularly the copper coil
Anticoagulant medications
Bleeding disorders (e.g. Von Willebrand disease)
Endocrine disorders (diabetes and hypothyroidism)
Connective tissue disorders
Endometrial hyperplasia or cance
Polycystic ovarian syndrome

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57
Q

What is post coital bleeding and why might it occur?

A

Postcoital bleeding (PCB) refers to bleeding after sexual intercourse. This is a red flag that should make you consider cervical and other cancers, although other causes are more common. Often no cause is found. The key causes are:

Cervical cancer, ectropion or infection
Trauma
Atrophic vaginitis
Polyps
Endometrial cancer
Vaginal cancer

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58
Q

What might cause pelvic pain?

A

Urinary tract infection
Dysmenorrhoea (painful periods)
Irritable bowel syndrome (IBS)
Ovarian cysts
Endometriosis
Pelvic inflammatory disease (infection)
Ectopic pregnancy
Appendicitis
Mittelschmerz (cyclical pain during ovulation)
Pelvic adhesions
Ovarian torsion
Inflammatory bowel disease (IBD)

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59
Q

Excessive, discoloured or foul-smelling discharge may indicate what?

A

Bacterial vaginosis
Candidiasis (thrush)
Chlamydia
Gonorrhoea
Trichomonas vaginalis
Foreign body
Cervical ectropion
Polyps
Malignancy
Pregnancy
Ovulation (cyclical)
Hormonal contraception

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60
Q

What is pruritus vulvae and why might it occur?

A

Pruritus vulvae refers to itching of the vulva and vagina

Irritants such as soaps, detergents and barrier contraception
Atrophic vaginitis
Infections such as candidiasis (thrush) and pubic lice
Skin conditions such as eczema
Vulval malignancy
Pregnancy-related vaginal discharge
Urinary or faecal incontinence
Stress

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61
Q

How is primary amenorrhoea definied?

A

Primary amenorrhoea is defined as not starting menstruation:

By 13 years when there is no other evidence of pubertal development
By 15 years of age where there are other signs of puberty, such as breast bud development

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62
Q

What is hypogonadism and what are the two reasons it might occur?

A

Hypogonadism refers to a lack of the sex hormones, oestrogen and testosterone, that normally rise before and during puberty. A lack of these hormones causes a delay in puberty. The lack of sex hormones is fundamentally due to one of two reasons:

Hypogonadotropic hypogonadism: a deficiency of LH and FSH
Hypergonadotropic hypogonadism: a lack of response to LH and FSH by the gonads (the testes and ovaries)

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63
Q

What is hypogonadotrophic hypogonadism?

A

Hypogonadotropic hypogonadism involves deficiency of LH and FSH, leading to deficiency of the sex hormones (oestrogen). LH and FSH are gonadotrophins produced by the anterior pituitary gland in response to gonadotropin releasing hormone (GnRH) from the hypothalamus. Since no gonadotrophins are simulating the ovaries, they do not respond by producing sex hormones (oestrogen). Therefore, “hypogonadotropism” causes “hypogonadism”.

A deficiency of LH and FSH is the result of abnormal functioning of the hypothalamus or pituitary gland. This could be due to:

Hypopituitarism (under production of pituitary hormones)
Damage to the hypothalamus or pituitary, for example, by radiotherapy or surgery for cancer
Significant chronic conditions can temporarily delay puberty (e.g. cystic fibrosis or inflammatory bowel disease)
Excessive exercise or dieting can delay the onset of menstruation in girls
Constitutional delay in growth and development is a temporary delay in growth and puberty without underlying physical pathology
Endocrine disorders such as growth hormone deficiency, hypothyroidism, Cushing’s or hyperprolactinaemia
Kallman syndrome

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64
Q

What is hypergonadotropic hypogonadism and why might occur?

A

Hypergonadotropic hypogonadism is where the gonads fail to respond to stimulation from the gonadotrophins (LH and FSH). Without negative feedback from the sex hormones (oestrogen), the anterior pituitary produces increasing amounts of LH and FSH. Consequently, you get high gonadotrophins (“hypergonadotropic”) and low sex hormones (“hypogonadism”).

Hypergonadotropic hypogonadism is the result of abnormal functioning of the gonads. This could be due to:

Previous damage to the gonads (e.g. torsion, cancer or infections such as mumps)
Congenital absence of the ovaries
Turner’s syndrome (XO)

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65
Q

What is Kallman syndrome?

A

Kallman syndrome is a genetic condition causing hypogonadotrophic hypogonadism, with failure to start puberty.

It is associated with a reduced or absent sense of smell (anosmia).

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66
Q

What is congenital adrenal hyperplasia and why might it occur?

A

Congenital adrenal hyperplasia is caused by a congenital deficiency of the 21-hydroxylase enzyme.

This causes underproduction of cortisol and aldosterone, and overproduction of androgens from birth. It is a genetic condition inherited in an autosomal recessive pattern. In a small number of cases, it involves a deficiency of 11-beta-hydroxylase rather than 21-hydroxylase.

In severe cases, the neonate is unwell shortly after birth, with electrolyte disturbances and hypoglycaemia. In mild cases, female patients can present later in childhood or at puberty with typical features:

Tall for their age
Facial hair
Absent periods (primary amenorrhoea)
Deep voice
Early puberty

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67
Q

What is androgen insensitivity syndrome?

A

Androgen insensitivity syndrome is a condition where the tissues are unable to respond to androgen hormones (e.g. testosterone), so typical male sexual characteristics do not develop. It results in a female phenotype, other than the internal pelvic organs.

Patients have normal female external genitalia and breast tissue. Internally there are testes in the abdomen or inguinal canal, and an absent uterus, upper vagina, fallopian tubes and ovaries.

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68
Q

Structural pathology resulting in primary amenorrhoea?

A

Structural pathology in the pelvic organs can prevent menstruation. If the ovaries are unaffected, there will be typical secondary sexual characteristics, but no menstrual periods. There may be cyclical abdominal pain as menses build up but are unable to escape through the vagina. Structural pathology that can cause primary amenorrhoea include:

Imperforate hymen
Transverse vaginal septae
Vaginal agenesis
Absent uterus
Female genital mutilation

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69
Q

When would primary amenorrhea be investigated?

A

The threshold for initiating investigations is no evidence of pubertal changes in a girl aged 13.

Investigation can also be considered when there is some evidence of puberty but no progression after two years.

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70
Q

How might primary amenorrhea be investigated?

A

BLOODS FOR UNDERLYING MEDICAL CONDITIONS

Full blood count and ferritin for anaemia

U&E for chronic kidney disease

Anti-TTG or anti-EMA antibodies for coeliac disease

BLOODS FOR HORMONAL ABNORMALITIES

FSH and LH (will be low in hypogonadotropic hypogonadism and high in hypergonadotropic hypogonadism)

Thyroid function tests

Insulin-like growth factor I is used as a screening test for GH deficiency

Prolactin (raised in hyperprolactinaemia)

Testosterone is raised in polycystic ovarian syndrome, androgen insensitivity syndrome and congenital adrenal hyperplasia

Genetic testing with a microarray test to assess for underlying genetic conditions:

Turner’s syndrome (XO)

IMAGING

Xray of the wrist to assess bone age and inform a diagnosis of constitutional delay

Pelvic ultrasound to assess the ovaries and other pelvic organs

MRI of the brain to look for pituitary pathology and assess the olfactory bulbs in possible Kallman syndrome

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71
Q

Primary Amenorrhoea - management

A

Management of primary amenorrhoea involves establishing and treating the underlying cause.

Where necessary, replacement hormones can induce menstruation and improve symptoms.

Patients with constitutional delay in growth and development may only require reassurance and observation.

Where the cause is due to stress or low body weight secondary to diet and exercise, treatment involves a reduction in stress, cognitive behavioural therapy and healthy weight gain.

Where the cause is due to an underlying chronic or endocrine condition, management involves optimising treatment for that condition.

In patients with hypogonadotrophic hypogonadism, such as hypopituitarism or Kallman syndrome, treatment with pulsatile GnRH can be used to induce ovulation and menstruation. This has the potential to induce fertility.

Alternatively, where pregnancy is not wanted, replacement sex hormones in the form of the combined contraceptive pill may be used to induce regular menstruation and prevent the symptoms of oestrogen deficiency.

In patients with an ovarian cause of amenorrhoea, such as polycystic ovarian syndrome, damage to the ovaries or absence of the ovaries, the combined contraceptive pill may be used to induce regular menstruation and prevent the symptoms of oestrogen deficiency.

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72
Q

What might cause primary amenorrhoea?

A

Constitutional delay in puberty

Chromosomal or genetic abnormalities such as Turner syndrome (45 XO) (gonadal dysgenisis) Kallmann syndrome and androgen insensitivity syndrome.

Disruption of the functioning of the hypothalamic or pituitary glands (functional hypothalamic amenorrhoea) For example as a result of:
- Anorexia and other eating disorders,
- Excessive exercise
- Extreme physical or psychological stress

Structural abnormalities of the genital tract such as:
- Imperforate hymen obstructing menstrual flow (leading to haematocolpos)
- Uterine agenesis
- Pregnancy

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73
Q

What is secondary amenorrhea? When should it be investigated?

A

Secondary amenorrhea is defined as no menstruation for more than three months after previous regular menstrual periods.

Consider assessment and investigation after three to six months.

In women with previously infrequent irregular periods, consider investigating after six to twelve months.

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74
Q

Causes of secondary amenorrhea?

A

Pregnancy is the most common cause

Menopause and premature ovarian failure

Hormonal contraception (e.g. IUS or POP)

Hypothalamic or pituitary pathology (hypothalamic amenorrhoea - (e.g. secondary stress, excessive exercise)),

Ovarian causes such as polycystic ovarian syndrome (androgen levels raised)

Uterine pathology such as Asherman’s syndrome (intrauterine adhesions)

Thyroid pathology (thyrotoxicosis, hypothyroidism)

Hyperprolactinaemia

Sheenans syndrome

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75
Q

Hypothalamic aetiology of secondary amenorrhoea?

A

The hypothalamus reduces the production of GnRH in response to significant physiological or psychological stress.

This leads to hypogonadotropic hypogonadism and amenorrhoea. The hypothalamus responds this way to prevent pregnancy in situations where the body may not be fit for it, for example:

Excessive exercise (e.g. athletes)
Low body weight and eating disorders
Chronic disease
Psychological stress

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76
Q

Pituitary causes of secondary amenorrhoea?

A

Pituitary causes of secondary amenorrhoea include:

Pituitary tumours, such as a prolactin-secreting prolactinoma
Pituitary failure due to trauma, radiotherapy, surgery or Sheehan syndrome

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77
Q

How can hyperprolactinemia cause secondary amenorrhea?
Why might it occur?
How is it managed?

A

High prolactin levels act on the hypothalamus to prevent the release of GnRH. Without GnRH, there is no release of LH and FSH.

This causes hypogonadotropic hypogonadism. Only 30% of women with a high prolactin level will have galactorrhea (breast milk production and secretion).

The most common cause of hyperprolactinaemia is a pituitary adenoma secreting prolactin. Where there are high prolactin levels, a CT or MRI scan of the brain is used to assess for a pituitary tumour.
Often there is a microadenoma that will not appear on the initial scan, and follow up scans are required to identify tumours that may develop later.

Often no treatment is required for hyperprolactinaemia.

Dopamine agonists such as bromocriptine or cabergoline can be used to reduce prolactin production

These medications treat hyperprolactinaemia, Parkinson’s disease and acromegaly.

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78
Q

How is secondary amenorrhoea investigated?

A

Detailed history and examination to assess for potential causes

Ultrasound of the pelvis to diagnose polycystic ovarian syndrome

Hormonal blood tests:
- Beta human chorionic gonadotropin (HCG) urine or blood tests (pregnancy)
-LH and FSH
- Prolactin (can be measured to assess for hyperprolactinaemia, followed by an MRI to identify a pituitary tumour)
- Thyroid stimulating hormone (TSH) (screen for thyroid pathology) This is followed by T3 and T4 when the TSH is abnormal)
- Testosterone: (Raise testosterone indicates polycystic ovarian syndrome, androgen insensitivity syndrome or congenital adrenal hyperplasia)

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79
Q

Interpreting abnormal FSH and LH in the context of secondary amenorrhea?

A

High FSH suggests primary ovarian failure

High LH, or LH:FSH ratio, suggests polycystic ovarian syndrome

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80
Q

What should you advise women taking hormonal replacement to manage PCOS to minimize risk and why?

A

Require a withdrawal bleed every 3 – 4 months to reduce the risk of endometrial hyperplasia and endometrial cancer.

Medroxyprogesterone for 14 days, or regular use of the combined oral contraceptive pill, can be used to stimulate a withdrawal bleed.

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81
Q

Management of secondary amenorrhea?

A

Management of secondary amenorrhoea involves establishing and treating the underlying cause. Where necessary, replacement hormones can induce menstruation and improve symptoms.

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82
Q

What non-gynecological condition can secondary amenorrhea increase the risk of, and when is treatment indicated to minimize this risk? What treatment is used?

A

Patients with amenorrhoea associated with low oestrogen levels are at risk increased risk of osteoporosis.

Where the amenorrhoea lasts more than 12 months, treatment is indicated to reduce the risk of osteoporosis:

Ensure adequate vitamin D and calcium intake
Hormone replacement therapy or the combined oral contraceptive pill

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83
Q

What is premenstural syndrome and why does it occur?

A

Premenstrual syndrome (PMS) describes the psychological, emotional and physical symptoms that occur during the luteal phase of the menstrual cycle, particularly in the days prior to the onset of menstruation. These symptoms can be distressing and significantly impact quality of life.

Most women will experience some of the symptoms of premenstrual syndrome. The critical aspects are the severity of the symptoms, and the impact these symptoms have on the woman’s functioning and quality of life.

The symptoms of PMS resolve once menstruation begins. Symptoms are not present before menarche, during pregnancy or after menopause. These are key things to note when you take a history.

Premenstrual syndrome is though to the caused by fluctuation in oestrogen and progesterone hormones during the menstrual cycle. The exact mechanism is not known, but it may be due to increased sensitivity to progesterone or an interaction between the sex hormones and the neurotransmitters serotonin and GABA.

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84
Q

How might PMS present?

A

There is a long list of symptoms that can occur with premenstrual syndrome, and these will vary with the individual. Common symptoms include:

Low mood
Anxiety
Mood swings
Irritability
Bloating
Fatigue
Headaches
Breast pain
Reduced confidence
Cognitive impairment
Clumsiness
Reduced libido
These symptoms can occur in the absence of menstruation after a hysterectomy, endometrial ablation or on the Mirena coil, as the ovaries continue to function and the hormonal cycle continues. They can also occur in response to the combined contraceptive pill or cyclical hormone replacement therapy containing progesterone, and this is described as progesterone-induced premenstrual disorder.

When features are severe and have a significant effect on quality of life, this is called premenstrual dysphoric disorder.

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85
Q

How is PMS diagnosed and managed?

A

Diagnosis is made based on a symptom diary spanning two menstrual cycles. The symptom diary should demonstrate cyclical symptoms that occur just before, and resolve after, the onset of menstruation. A definitive diagnosis may be made, under the care of a specialist, by administering a GnRH analogues to halt the menstrual cycle and temporarily induce menopause, to see if the symptoms resolve.

The following management options can be initiated in primary care:

General healthy lifestyle changes, such as improving diet, exercise, alcohol, smoking, stress and sleep
Combined contraceptive pill (COCP)
SSRI antidepressants
Cognitive behavioural therapy (CBT)
RCOG recommends COCPs containing drospirenone first line (i.e. Yasmin). Drospironone as some antimineralocortioid effects, similar to spironolactone. Continuous use of the pill, as opposed to cyclical use, may be more effective.

Severe cases should be managed by a multidisciplinary team, involving GPs, gynaecologists, psychologists and dieticians.

Continuous transdermal oestrogen (patches) can be used to improve symptoms. Progestogens are required for endometrial protection against endometrial hyperplasia when using oestrogen. This can be in the form of low dose cyclical progestogens (e.g. norethisterone) to trigger a withdrawal bleed, or the Mirena coil.

GnRH analogues can be used to induce a menopausal state. They are very effective at controlling symptoms; however, they are reserved for severe cases due to the adverse effects (e.g. osteoporosis). Hormone replacement therapy can be used to add back the hormones to mitigate these effects.

Hysterectomy and bilateral oophorectomy can be used to induce menopause where symptoms are severe and medical management has failed. Hormone replacement therapy will be required, particularly in women under 45 years.

Danazole and tamoxifen are options for cyclical breast pain, initiated and monitored by a breast specialist.

Spironolactone may be used to treat the physical symptoms of PMS, such as breast swelling, water retention and bloating.

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86
Q

Types of Fibroids

A

Intramural: within the myometrium (the muscle of the uterus). As they grow, they change the shape and distort the uterus.

Subserosal means (just below the outer layer of the uterus) These fibroids grow outwards and can become very large, filling the abdominal cavity.

Submucosal (just below endometirum)

Pedunculated (on a stalk)

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87
Q

How might fibroids present?

A

Fibroids are often asymptomatic. They can present in several ways:

Heavy menstrual bleeding (menorrhagia) is the most frequent presenting symptom
Prolonged menstruation, lasting more than 7 days
Abdominal pain, worse during menstruation
Bloating or feeling full in the abdomen
Urinary or bowel symptoms due to pelvic pressure or fullness
Deep dyspareunia (pain during intercourse)
Reduced fertility
Abdominal and bimanual examination may reveal a palpable pelvic mass or an enlarged firm non-tender uterus.

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88
Q

How can fibroids be investigated?

A

Hysteroscopy is the initial investigation for submucosal fibroids presenting with heavy menstrual bleeding.

Pelvic ultrasound is the investigation of choice for larger fibroids.

MRI scanning may be considered before surgical options, where more information is needed about the size, shape and blood supply of the fibroids.

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89
Q

How are fibroids over 3cm managed?

A

For fibroids less than 3 cm, the medical management is the same as with heavy menstrual bleeding:

Mirena coil (1st line) – fibroids must be less than 3cm with no distortion of the uterus
Symptomatic management with NSAIDs and tranexamic acid
Combined oral contraceptive
Cyclical oral progestogens

Surgical options for managing smaller fibroids with heavy menstrual bleeding are:

Endometrial ablation
Resection of submucosal fibroids during hysteroscopy
Hysterectomy

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90
Q

Over what side fibroid does a woman need referral to gynecology for investigation and management?

A

3 cm

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91
Q

How are fibroids over 3cm managed?

A

For fibroids more than 3 cm, women need referral to gynaecology for investigation and management. Medical management options are:

Symptomatic management with NSAIDs and tranexamic acid (antifibrinolytics)
Mirena coil – depending on the size and shape of the fibroids and uterus
Combined oral contraceptive
Cyclical oral progestogens

Surgical options for larger fibroids are:

Uterine artery embolisation (may preserve fertility)
Myomectomy (usually preserves fertility)
Hysterectomy
Radio frequency ablation to induce necrosis of the fibroid

GnRH agonists, such as goserelin (Zoladex) or leuprorelin (Prostap), may be used to reduce the size of fibroids before surgery. They work by inducing a menopause-like state and reducing the amount of oestrogen maintaining the fibroid. Usually, GnRH agonists are only used short term, for example, to shrink a fibroid before myomectomy.

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92
Q

What is uterine artery embolisation?

A

Uterine artery embolisation is a surgical option for larger fibroids, performed by interventional radiologists.

The radiologist inserts a catheter into an artery, usually the femoral artery. This catheter is passed through to the uterine artery under X-ray guidance. Once in the correct place, particles are injected that cause a blockage in the arterial supply to the fibroid.

This starves the fibroid of oxygen and causes it to shrink.

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93
Q

Surgical management of fibroids

A

Myomectomy involves surgically removing the fibroid via laparoscopic (keyhole) surgery or laparotomy (open surgery). Myomectomy is the only treatment known to potentially improve fertility in patients with fibroids.

Endometrial ablation can be used to destroy the endometrium. Second generation, non-hysteroscopic techniques are used, such as balloon thermal ablation. This involves inserting a specially designed balloon into the endometrial cavity and filling it with high-temperature fluid that burns the endometrial lining of the uterus.

Hysterectomy involves removing the uterus and fibroids. Hysterectomy may be by laparoscopy (keyhole surgery), laparotomy or vaginal approach. The ovaries may be removed or left depending on patient preference, risks and benefits.

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94
Q

What treatment can improve fertility in patients with fibroids?

A

Myomectomy

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95
Q

What are the potential complications of fibroids?

A

Heavy menstrual bleeding, often with iron deficiency anaemia

Reduced fertility

Pregnancy complications, such as miscarriages, premature labour and obstructive delivery

Constipation

Urinary outflow obstruction and urinary tract infections

Red degeneration of the fibroid

Torsion of the fibroid, usually affecting pedunculated fibroids

Malignant change to a leiomyosarcoma is very rare (<1%)

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96
Q

What is red degeneration of the fibroid?

A

Ischaemia, infarction and necrosis of the fibroid due to disrupted blood supply.

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97
Q

Which fibroids are more likely to undergo red degeneration?

A

Red degeneration is more likely to occur in larger fibroids (above 5 cm) during the second and third trimester of pregnancy.

Red degeneration may occur as the fibroid rapidly enlarges during pregnancy, outgrowing its blood supply and becoming ischaemic.

It may also occur due to kinking in the blood vessels as the uterus changes shape and expands during pregnancy.

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98
Q

How does red degeneration of a fibroid present?

A

Red degeneration presents with severe abdominal pain, low-grade fever, tachycardia and often vomiting.

Management is supportive, with rest, fluids and analgesia.

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99
Q

What is the likely diagnosis for a pregnant woman with a history of fibroids presenting with severe abdominal pain and a low-grade fever

A

Red degeneration of a fibroid

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100
Q

What is endometriosis?

A

Endometriosis is a condition where there is ectopic endometrial tissue outside the uterus.

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101
Q

A lump of endometrial tissue outside the uterus is described what?

A

as an endometrioma.

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102
Q

Endometriomas in the ovaries are often called what?

A

“chocolate cysts”.

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103
Q

What term refers to endometrial tissue within the myometrium (muscle layer) of the uterus.

A

Adenomyosis refers to endometrial tissue within the myometrium (muscle layer) of the uterus.

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104
Q

Aetiology of endometriosis?

A

The exact cause of endometriosis is not clear, but there are several theories.

No specific genes have been found to cause endometriosis; however, there does seem to be a genetic component to developing the condition.

One notable theory for the cause of ectopic endometrial tissue is that during menstruation, the endometrial lining flows backwards, through the fallopian tubes and out into the pelvis and peritoneum.
This is called retrograde menstruation.
The endometrial tissue then seeds itself around the pelvis and peritoneal cavity.

Other possible methods for endometrial tissue exiting the uterus have been proposed:

  • Embryonic cells destined to become endometrial tissue may remain in areas outside the uterus during the development of the fetus, and later develop into ectopic endometrial tissue.
  • There may be spread of endometrial cells through the lymphatic system, in a similar way to the spread of cancer.
  • Cells outside the uterus somehow change, in a process called metaplasia, from typical cells of that organ into endometrial cells.
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105
Q

Pathophysiology of symptoms in endometriosis?

A

CYCLICAL PAIN - DULL, HEAVY BURNING PAIN:
Endometrial tissue outside the uterus responds to hormones in the same way as endometrial tissue in the uterus. It bleeds during menstruation as it sheds (the same way it does in the uterus) causing irritation and inflammation of the surrounding tissues.

BLOOD IN URINE AND STOOLS
Endometrium deposits in the bowel or bladder

CHRONIC NON-CYCLICAL PAIN - SHARP, STABBING OR PULLING PAIN ASSOCIATED WITH NAEUSEA:
Adhesions form from localised bleeding and inflammation. Scar tissue binds organs together (e.g. ovaries to peritoneum, uterus to bowel)

REDUCED FERTILITY:
Unclear - may be due to adhesions around the ovaries and fallopian tubes blocking the release of eggs or kinking the fallopian tubes obstructing the route to the uterus. Endometriomas in the ovaries may also damage eggs or prevent effective ovulation.

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106
Q

How might endometriosis present?

A

Asymptomatic

Cyclical: abdominal or pelvic pain, urinary symptoms and bowel symptoms

Deep dyspareunia (pain on deep sexual intercourse)

Dysmenorrhea (painful periods)

Infertility

Cyclical bleeding from other sites such as haematuria

O/E: Endometrial tissue visable in the bagina and on speculum examination, particularly in the posterior fornix, a fixed cervix on bimanual examination, tenderness in the vagina, cervic and adnexa

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107
Q

Endometriosis O/E?

A

Endometrial tissue visible in the vagina on speculum examination, particularly in the posterior fornix

A fixed cervix on bimanual examination

Tenderness in the vagina, cervix and adnexa

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108
Q

How is endometriosis diagnosis?

A

Pelvic ultrasound may reveal large endometriomas and chocolate cysts. Ultrasound scans are often unremarkable in patients with endometriosis. Patients with suspected endometriosis need referral to a gynaecologist for laparoscopy.

Laparoscopic surgery is the gold standard way to diagnose abdominal and pelvic endometriosis. A definitive diagnosis can be established with a biopsy of the lesions during laparoscopy. Laparoscopy has the added benefit of allowing the surgeon to remove deposits of endometriosis and potentially improve symptoms.

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109
Q

How is endometreosis staged?

A

American Society of Reproductive Medicine (ASRM)

Stage 1: Small suoerficial lesions
Stage 2 Mild but deeper lesions than stage 1
Stage 3: Deeper lesion with lesions on the ovaries and mild adhesions
Stage 4: Deep and large lesions affecting the ovaries with extensive adhesions

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110
Q

Existing guidlines fo endometriosis management

A

RCOG Green-top guideline 41 on chronic pelvic pain (2012), the ESHRE guidelines on endometriosis (2013) and the NICE clinical knowledge summaries (2020).

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111
Q

What does initial management of endometriosis involve?

A

Establishing a diagnosis
Proving a clear explanation
Listening to the patient establishing ICE and building a partnership
Analgesia as required for pain (NSAIDs and paracetomol first line)

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112
Q

When can hormonal management options for endometresosis be tried and what are they?

A

Hormonal management options can be tried before establishing a definitive diagnosis with laparoscopy:

Combined oral contractive pill, which can be used back to back without a pill-free period if helpful
Progesterone only pill
Medroxyprogesterone acetate injection (e.g. Depo-Provera)
Nexplanon implant
Mirena coil
GnRH agonists

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113
Q

What treatment of endometriosis may improve fertility?

A

Laparoscopic surgery to excise or ablate the endometrial tissue and remove adhesions (adhesiolysis)
The aim is to remove as much of the endometriosis as possible, treat adhesions and return the anatomy to normal. This improves fertility in some but not all women with endometriosis.

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114
Q

Surgical management of endometriosis

A

Laparoscopic surgery to excise or ablate the endometrial tissue and remove adhesions (adhesiolysis)
Hysterectomy
Laparoscopic treatment may improve fertility. Hormonal therapies may improve symptoms but not fertility.

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115
Q

What therapy can treat cyclical pain in endometriosis?

A

Cyclical pain can be treated with hormonal medications that stop ovulation and reduce endometrial thickening. This can be achieved using the combined oral contraceptive pill, oral progesterone-only pill, the progestin depot injection, the progestin implant (Nexplanon) and the Mirena coil.

The cyclical pain tends to improve after the menopause when the female sex hormones are reduced. Therefore, another treatment option for endometriosis is to induce a menopause-like state using GnRH agonists. Examples of GnRH agonists are goserelin (Zoladex) or leuprorelin (Prostap). They shut down the ovaries temporarily and can be useful in treating pain in many women. However, inducing the menopause has several side effects, such as hot flushes, night sweats and a risk of osteoporosis.

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116
Q

What is the final surgical option to manage endometriosis?

A

Hysterectomy and bilateral salpingo-opherectomy is the final surgical option. During the procedure, the surgeon will attempt to remove as much of the endometriosis as possible. Importantly, this is still not guaranteed to resolve symptoms. Removing the ovaries induces menopause, and this stops ectopic endometrial tissue responding to the menstrual cycle

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117
Q

Adenomyosis

A

Adenomyosis refers to endometrial tissue inside the myometrium (muscle layer of the uterus).

It is more common in later reproductive years and those that have had several pregnancies (multiparous). It occurs in around 10% of women overall.

It may occur alone, or alongside endometriosis or fibroids. The cause is not fully understood, and multiple factors are involved, including sex hormones, trauma and inflammation. The condition is hormone-dependent, and symptoms tend to resolve after menopause, similarly to endometriosis and fibroids.

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118
Q

How does pregnancy hx relate to risk of adenomyosis?

A

Increased risk in multiparity

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119
Q

Cyclical vs non cyclical pain characteristics in endometriosis

A

NON CYCLICAL = sharp, stabbing or pulling associated with nausea?
Adhesions lead to a chronic, non-cyclical pain that can be sharp, stabbing or pulling and associated with nausea.

CYCLICAL = dull, heavy, burning pain
The cells of the endometrial tissue outside the uterus respond to hormones in the same way as endometrial tissue in the uterus during menstruation and shed as the endometrial tissue in the uterus sheds its lining and bleeds. This causes irritation and inflammation of the tissues around the sites of endometriosis. This results in the cyclical, dull, heavy or burning pain that occurs during menstruation in patients with endometriosis.

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120
Q

Presentation of adenomyosis

A

Adenomyosis typically presents with:

Painful periods (dysmenorrhoea)
Heavy periods (menorrhagia)
Pain during intercourse (dyspareunia)
It may also present with infertility or pregnancy-related complications. Around a third of patients are asymptomatic.

Examination can demonstrate an enlarged and tender uterus. It will feel more soft than a uterus containing fibroids.

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121
Q

How is adenomyosis diagnosed?

A

Transvaginal ultrasound of the pelvis is the first-line investigation for suspected adenomyosis.

MRI and transabdominal ultrasound are alternative investigations where transvaginal ultrasound is not suitable.

The gold standard is to perform a histological examination of the uterus after a hysterectomy. However, this is not usually a suitable way of establishing the diagnosis for obvious reasons.

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122
Q

How is adenomyosis managed?

A

Management of adenomyosis will depend on symptoms, age and plans for pregnancy. NICE recommend the same treatment for adenomyosis as for heavy menstrual bleeding.

When the woman does not want contraception; treatment can be used during menstruation for symptomatic relief, with:

Tranexamic acid when there is no associated pain (antifibrinolytic – reduces bleeding)
Mefenamic acid when there is associated pain (NSAID – reduces bleeding and pain)
Management when contraception is wanted or acceptable:

Mirena coil (first line)
Combined oral contraceptive pill
Cyclical oral progestogens
Progesterone only medications such as the pill, implant or depot injection may also be helpful.

Other options are that may be considered by a specialist include:

GnRH analogues to induce a menopause-like state
Endometrial ablation
Uterine artery embolisation
Hysterectomy

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123
Q

Adenomyosis - complications/associations

A

Infertility
Miscarriage
Preterm birth
Small for gestational age
Preterm premature rupture of membranes
Malpresentation
Need for caesarean section
Postpartum haemorrhage

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124
Q

What is menopause

A

Retrospective diagnosis of the end of mensturation

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125
Q

What is postmenopause

A

Postmenopause describes the period from 12 months after the final menstrual period onwards.

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126
Q

What is perimenopause

A

Perimenopause refers to the time around the menopause, where the woman may be experiencing vasomotor symptoms and irregular periods. Perimenopause includes the time leading up to the last menstrual period, and the 12 months afterwards. This is typically in women older than 45 years.

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127
Q

Before what age is menopause considered premature?

A

Premature menopause is menopause before the age of 40 years. It is the result of premature ovarian insufficiency.

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128
Q

What causes menopause?

A

Menopause is caused by a lack of ovarian follicular function, resulting in changes in the sex hormones associated with the menstrual cycle:

Oestrogen and progesterone levels are low
LH and FSH levels are high, in response to an absence of negative feedback from oestrogen

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129
Q

What is the physiology of menopause?

A

Decline in development of ovarian follicles

Due to this decrease development there is reduced production of oestrogen by the follicles

The decreased production of oestrogen results in decreased negative feedback on the pituitary gland, therefore more LH and FSH are produced.

As the level of oestrogen falls in the perimenopausal period, there is an absence of negative feedback on the pituitary gland, and increasing levels of LH and FSH.

The failing follicular development means ovulation does not occur (anovulation), resulting in irregular menstrual cycles.

Without oestrogen, the endometrium does not develop, leading to a lack of menstruation (amenorrhoea).

Lower levels of oestrogen also cause the perimenopausal symptoms.

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130
Q

A lack of oestrogen in the perimenopausal period leads to what symptoms?

A

Hot flushes
Emotional lability or low mood
Premenstrual syndrome
Irregular periods
Joint pains
Heavier or lighter periods
Vaginal dryness and atrophy
Reduced libido

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131
Q

What are post-menopausal women at increased risk of?

A

A lack of oestrogen increases the risk of certain conditions:

Cardiovascular disease and stroke
Osteoporosis
Pelvic organ prolapse
Urinary incontinence

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132
Q

In which patients is perimenopause a clinical diagnosis?

A

A diagnosis of perimenopause and menopause can be made in women over 45 years with typical symptoms, without performing any investigations.

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133
Q

NICE guidelines (2015) recommend considering an FSH blood test to help with the diagnosis of menopause in which patients?

A

Women under 40 years with suspected premature menopause
Women aged 40 – 45 years with menopausal symptoms or a change in the menstrual cycle

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134
Q

Fertility gradually declines after 40 years of age. However, women should still consider themselves fertile. Pregnancy after 40 is associated with increased risks and complications. Post menopausal women need to use effective contraception for how long after their last menstural period?

A

Two years after the last menstrual period in women under 50
One year after the last menstrual period in women over 50

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135
Q

Why is it difficult to diagnose women on hormonal contraceptives with menopause?

A

Hormonal contraceptives do not affect the menopause, when it occurs or how long it lasts, although they may suppress and mask the symptoms. This can make diagnosing menopause in women on hormonal contraception more difficult.

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136
Q

What are some good contraceptive options (UKMEC 1) for women approaching the menopause?

A

Barrier methods
Mirena or copper coil
Progesterone only pill
Progesterone implant
Progesterone depot injection (under 45 years)
Sterilisation

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137
Q

At what age does the COCP become UKMEC 2 (the advantages generally outweigh the risks) ?

A

after 40

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138
Q

Up to what age can the COCP be if there are no other contraindications?

A

50 YEARS

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139
Q

In women over 40 taking the COCP pills containing what should be considered and why?

A

Consider combined oral contraceptive pills containing norethisterone or levonorgestrel in women over 40, due to the relatively lower risk of venous thromboembolism compared with other options.

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140
Q

Why is the progesterone depo injection unsuitable in women over 40?

A

Two key side effects of the progesterone depot injection (e.g. Depo-Provera): weight gain and reduced bone mineral density (osteoporosis).

These side effects are unique to the depot and do not occur with other forms of contraception.

Reduced bone mineral density makes the depot unsuitable for women over 45 years.

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141
Q

Perimenopausal symtpoms management

A

No treatment
Hormone replacement therapy (HRT)
Tibolone, a synthetic steroid hormone that acts as continuous combined HRT (only after 12 months of amenorrhoea)
Clonidine, which act as agonists of alpha-adrenergic and imidazoline receptors
Cognitive behavioural therapy (CBT)
SSRI antidepressants, such as fluoxetine or citalopram
Testosterone can be used to treat reduced libido (usually as a gel or cream)
Vaginal oestrogen cream or tablets, to help with vaginal dryness and atrophy (can be used alongside systemic HRT)
Vaginal moisturisers, such as Sylk, Replens and YES

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142
Q

After how long will vasomotor perimenopausal symptoms resolve without any treatment?

A

2-5 years

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143
Q

What is premature ovarian insufficiency and why might it occur?

A

Premature ovarian insufficiency is defined as menopause before the age of 40 years.

It is the result of a decline in the normal activity of the ovaries at an early age.

It presents with early onset of the typical symptoms of the menopause.

Premature ovarian insufficiency is characterised by hypergonadotropic hypogonadism. Under-activity of the gonads (hypogonadism) means there is a lack of negative feedback on the pituitary gland, resulting in an excess of the gonadotropins (hypergonadotropism).

Hormonal analysis will show:

Raised LH and FSH levels (gonadotropins)
Low oestradiol levels

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144
Q

Causes of premature ovarian insufficency?

A

Idiopathic (the cause is unknown in more than 50% of cases)

Iatrogenic, due to interventions such as chemotherapy, radiotherapy or surgery (i.e. oophorectomy)

Autoimmune, possibly associated with coeliac disease, adrenal insufficiency, type 1 diabetes or thyroid disease

Genetic, with a positive family history or conditions such as Turner’s syndrome

Infections such as mumps, tuberculosis or cytomegalovirus

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145
Q

What will hormonal analysis show in premature ovarian insufficiency?

A

Hormonal analysis will show:

Raised LH and FSH levels (gonadotropins)
Low oestradiol levels

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146
Q

How does premature ovarian insufficiency present?

A

Premature ovarian insufficiency presents with irregular menstrual periods, lack of menstrual periods (secondary amenorrhea) and symptoms of low oestrogen levels, such has hot flushes, night sweats and vaginal dryness.

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147
Q

How is premature ovarian insufficiency diagnosed?

A

NICE guidelines on menopause (2015) say premature ovarian insufficiency can be diagnosed in women younger than 40 years with typical menopausal symptoms plus elevated FSH.

The FSH level needs to be persistently raised (more than 25 IU/l) on two consecutive samples separated by more than four weeks to make a diagnosis. The results are difficult to interpret in women taking hormonal contraception.

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148
Q

Women with premature ovarian insufficiency are at higher risk of conditions associated with low oesterogen, such as what?

A

Cardiovascular disease
Stroke
Osteoporosis
Cognitive impairment
Dementia
Parkinsonism

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149
Q

Management of premature ovarian insufficiency?

A

Management involves hormone replacement therapy (HRT) until at least the age of 51

HRT reduces the cardiovascular, osteoporosis, cognitive and psychological risks associated with premature menopause.

It is worth noting there is still a small risk of pregnancy in women with premature ovarian failure, and contraception is still required.

There are two options for HRT in women with premature ovarian insufficiency:

Traditional hormone replacement therapy

Combined oral contraceptive pill

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150
Q

HRT vs COCP in managing premature ovarian failure symptoms?

A

Traditional hormone replacement therapy is associated with a lower blood pressure compared with the combined oral contraceptive pill.

The combined pill may be more socially acceptable (less stigma for younger women) and additionally acts as contraception.

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151
Q

HRT associated breast cancer risk when used to manage premature ovarian insufficiency?

A

Hormone replacement therapy before the age of 50 is not considered to increase the risk of breast cancer compared with the general population, as women would ordinarily produce the same hormones at this age.

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152
Q

There may be an increased risk of venous thromboembolism with HRT in women under 50 years, how can this risk be reduced?

A

The risk of VTE can be reduced by using transdermal methods (i.e. patches).

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153
Q

What hormones are involved in HRT and what is their purpose?

A

Exogenous oestrogen is given to alleviate the symptoms associated with the decline in oestrogen levels during menopause and peri-menopause

Progesterone needs to be given (in addition to oestrogen) to women that have a uterus. The primary purpose of adding progesterone is to prevent endometrial hyperplasia and endometrial cancer secondary to “unopposed” oestrogen.

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154
Q

What is the purpose of progesterone in HRT and which women do not need it?

A

Prevents endometrial hyperplasia and endometrial cancer secondary to unopposed oestrogen

Only required for women who have a uterus

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155
Q

What type of HRT regime should women that still have periods go on?

A

Women that still have periods should go on cyclical HRT, with cyclical progesterone and regular breakthrough bleeds.

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156
Q

Postmenopausal women with a uterus and more than 12 months without periods should go on what HRT regime?

A

Postmenopausal women with a uterus and more than 12 months without periods should go on continuous combined HRT.

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157
Q

Non-hormonal management of menopause (HRT alternatives)

A

Non-hormonal treatments may be tried initially, or used when there are contraindications to HRT. Options include:

Lifestyle changes such as improving the diet, exercise, weight loss, smoking cessation, reducing alcohol, reducing caffeine and reducing stress

Cognitive behavioural therapy (CBT)

Clonidine, which is an agonist of alpha-adrenergic and imidazoline receptors

SSRI antidepressants (e.g. fluoxetine)

Venlafaxine, which is a selective serotonin-norepinephrine reuptake inhibitor (SNRI)

Gabapentin

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158
Q

Clonidine may be used instead of HRT, how does it work and what side effects may occur?

A

Clonidine act as an agonist of alpha-2 adrenergic receptors and imidazoline receptors in the brain.

It lowers blood pressure and reduces the heart rate, and is also used as an antihypertensive medication.

It can be helpful for vasomotor symptoms and hot flushes, particularly where there are contraindications to using HRT.

Common side effects of clonidine are dry mouth, headaches, dizziness and fatigue.

Sudden withdrawal can result in rapid increases in blood pressure and agitation.

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159
Q

What herbal remedies might patients try to manage menopause and what problems might they cause?

A

Black cohosh, which may be a cause of liver damage

Dong quai, which may cause bleeding disorders

Red clover, which may have oestrogenic effects that would be concerning with oestrogen sensitive cancers

Evening primrose oil, which has significant drug interactions and is linked with clotting disorders and seizures

Ginseng may be used for mood and sleep benefits

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160
Q

What are the indications for HRT?

A

Replacing hormones in premature ovarian insufficiency, even without symptoms

Reducing vasomotor symptoms such as hot flushes and night sweats

Improving symptoms such as low mood, decreased libido, poor sleep and joint pain

Reducing risk of osteoporosis in women under 60 years

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161
Q

Benefits of HRT?

A

In women under 60 years, the benefits of HRT generally outweigh the risks.

The key benefits to inform women of include:

Improved vasomotor and other symptoms of menopause (including mood, urogenital and joint symptoms)
Improved quality of life
Reduced the risk of osteoporosis and fractures

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162
Q

The risks of HRT are more significant in older women and increase with a longer duration of treatment.

The principal risks of HRT are what?

A

Increased risk of breast cancer (particularly combined HRT – oestrogen-only HRT has a lower risk)

Increased risk of endometrial cancer

Increased risk of venous thromboembolism (2 – 3 times the background risk)

Increased risk of stroke and coronary artery disease with long term use in older women

The evidence is inconclusive about ovarian cancer, and if there is an increase in risk, it is minimal

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163
Q

In which patients do certain risks associated with HRT apply to?

A

The risks are not increased in women under 50 years compared with other women their age

There is no risk of endometrial cancer in women without a uterus

There is no increased risk of coronary artery disease with oestrogen-only HRT (the risk may even be lower with HRT)

164
Q

How to reduce endometrial cancer risk associated with HRT?

A

The risk of endometrial cancer is greatly reduced by adding progesterone in women with a uterus

165
Q

How to reduce VTE risk associated with HRT?

A

The risk of VTE is reduced by using patches rather than pills

166
Q

Essentiel contraindications to HRT?

A

Undiagnosed abnormal bleeding

Endometrial hyperplasia or cancer

Breast cancer

Uncontrolled hypertension

Venous thromboembolism

Liver disease

Active angina or myocardial infarction

Pregnancy

167
Q

What should be checked and considered prior to starting HRT?

A

Take a full history to ensure there are no contraindications

Take a family history to assess the risk of oestrogen dependent cancers (e.g. breast cancer) and VTE

Check the body mass index (BMI) and blood pressure

Ensure cervical and breast screening is up to date

Encourage lifestyle changes that are likely to improve symptoms and reduce risks

168
Q

Three steps to consider when choosing HRT forumlation?

A
  1. LOCAL OR SYSTEMIC SYMPTOMS

Local symptoms: use topical treatments such as topical oestrogen cream or tablets
Systemic symptoms: use systemic treatment – go to step 2

  1. UTERUS OR NON UTERUS

No uterus: use continuous estrogen-only HRT
Has uterus: add progesterone (combined HRT) – go to step 3

  1. BLEED IN LAST 12 MONTHS?

Perimenopausal: give cyclical combined HRT
Postmenopausal (more than 12 months since last period): give continuous combined HRT

169
Q

HRT: options for oestrogen delivery?

A

Oestrogen is the critical component of HRT for reducing the symptoms of menopause.

There are two options for delivering systemic oestrogen:
- Oral (tablets)
- Transdermal (patches or gels)

Patches are more suitable for women with poor control on oral treatment, higher risk of venous thromboembolism, cardiovascular disease and headaches.

170
Q

HRT: options for progesterone delivery?

A

There are three options for delivering progesterone for endometrial protection:

  1. Oral (tablets)
  2. Transdermal (patches)
  3. Intrauterine system (e.g. Mirena coil)

Cyclical combined HRT options include sequential tablets or patches containing continuous oestrogen with progesterone added for specific periods during the cycle.

The Mirena coil is licensed for four years for endometrial protection, after which time it needs replacing. The Mirena coil has the added benefits of contraception and treating heavy menstrual periods. It can cause irregular bleeding and spotting in the first few months after insertion. This usually settles with time and many women become amenorrhoeic.

171
Q

Causes of secondary dysmenorrhoea

A

endometriosis
adenomyosis
pelvic inflammatory disease
intrauterine devices*
fibroids

172
Q

Primary vs secondary dysmenorrhoea

A

In primary dysmenorrhoea there is no underlying pelvic pathology. It affects up to 50% of menstruating women and usually appears within 1-2 years of the menarche. Excessive endometrial prostaglandin production is thought to be partially responsible.

Features
pain typically starts just before or within a few hours of the period starting
suprapubic cramping pains which may radiate to the back or down the thigh

Secondary dysmenorrhoea typically develops many years after the menarche and is the result of an underlying pathology. In contrast to primary dysmenorrhoea the pain usually starts 3-4 days before the onset of the period.

173
Q

Endometriosis: typical PV EXAMINATION

A

On examination, you find that the patient is mildly overweight; her abdomen is soft
with no obvious masses. On vaginal examination you find a normal-sized, fixed
retroverted uterus, and there is tenderness in the posterior vaginal fornix. Both
adnexa appear normal.

174
Q

First line investigation for fibroids?

A

Transvaginal ultrasound

175
Q

Most communal cause of post menopausal bleeding

A

Vaginal atrophy

176
Q

Most common type of ovarian cyst?

A

Functional type - follicular

177
Q

Types of functional cysts

A

Follicular (most common)
Corpus leuteum cyst (usually seen in early pregnancy when corpus leuteum fails to break down)

178
Q

Ovarian cyst rupture presentation

A

Sudden onset abdominal pain typically occuring during exercise

179
Q

What compressive symptoms can fibroids cause?

A

Urinary frequency
Constipation
Pedal odema

180
Q

Dysmenorrhoea is uncommon in fibroids, but why might it occur?

A

Red degeneration of the fibroid (haemorrhage into the fibroid)
Sarcomatous change
Torsion of the fibroid

181
Q

Obstetric common P/C

A

N&V - hyperemisis gravidarum
Abnormal vaginal discharge including bleeding, watery
Reduced feotal movement after 20 weeks gestation

182
Q

What is a rectocele?

A

Rectum prolapses into the vagina due to a defect in the posterior vaginal wall

183
Q

Speculum examination: insertion

A

Use lubricant and warm speculum

Hold speculum in dominant hand

Part labia with nondominant hand

Slowly insert and open speculum blades to visualize the cervix

184
Q

How to perform a bimanual examination

A

Separate labia with gloved left hand

Slowly insert index finger and middle finger into vagina and palpate the cervix

Left hand then palpates uterus and adnexa abdominally

185
Q

What organism is usually responsible for infection of a Bartholin’s cyst?

A

Escherichia coli

186
Q

What is a bartholin’s cyst?

A

Bartholin’s glands are situated within the vestibule, just lateral to the introitus and normally function to secrete a lubricating fluid.

Bartholin’s gland cyst: occurs when the duct from the gland becomes blocked, resulting in palpable swelling and pain at the site of the Bartholin’s gland

187
Q

What is a nabothian cyst?

A

Nabothian cysts are cysts on the cervix that occur when the squamous-cell epithelium of the cervix slightly covers the columnar epithelium.

As the columnar epithelium secretes mucous, the mucous becomes trapped, and cysts form.

The cysts contain yellow/amber mucous and are usually located around the os where the epitheliums transition. They are a normal finding, particularly in women who have had children.

188
Q

What is the whirlpool sign on CT

A

The ‘Whirlpool’ sign is a characteristic sign of ovarian torsion that can be seen on ultrasound or CT scan. It demonstrates the twisting of the ovarian pedicle

189
Q

A history of aching, fullness and bloating in a young woman are typical symptoms of what?

A

An ovarian cyst

190
Q

NICE recommends the consideration of SSRIs where premenstrual syndrome is severe. When can they be taken?

A

These can be taken during the luteal phase of the menstrual cycle (days 15–28).

191
Q

Common causes of pelvic inflammatory disease?

A

Chlamydia trachomatis or Neisseria gonorrhoeae

192
Q

What is pelvic organ prolapse the result of?

A

Prolapse is the result of weakness and lengthening of the ligaments and muscles surrounding the uterus, rectum and bladder.

192
Q

What is pelvic organ prolapse the result of?

A

Weakness and lengthening of the ligaments and muscles surrounding the uterus, rectum and bladder.

193
Q

What is uterine prolapse?

A

Uterine prolapse is where the uterus itself descends into the vagina.

194
Q

What is vault prolapse?

A

Vault prolapse occurs in women that have had a hysterectomy, and no longer have a uterus. The top of the vagina (the vault) descends into the vagina.

195
Q

What are rectoceles?

A

Rectoceles are caused by a defect in the posterior vaginal wall, allowing the rectum to prolapse forwards into the vagina.

196
Q

What are rectoceles associated with, and what problems can they cause?

A

Rectoceles are particularly associated with constipation. Women can develop faecal loading in the part of the rectum that has prolapsed into the vagina. Loading of faeces results in significant constipation, urinary retention (due to compression on the urethra) and a palpable lump in the vagina.

197
Q

How can a rectocele be manipulated by the patient to allow passage of feaces?

A

Women may use their fingers to press the lump backwards, correcting the anatomical position of the rectum, and allowing them to open their bowels.

198
Q

What are cystoceles?

A

Cystoceles are caused by a defect in the anterior vaginal wall, allowing the bladder to prolapse backwards into the vagina.

199
Q

What is a urethrocele

A

Prolapse of the urethra

200
Q

What is a cystourethrocele?

A

Prolapse of both the bladder and the urethra

201
Q

What are risk factors for pelvic organ prolapse?

A

Multiple vaginal deliveries

Instrumental, prolonged or traumatic delivery

Advanced age and postmenopause status

Obesity

Chronic respiratory disease causing coughing

Chronic constipation causing straining

202
Q

How might pelvic organ prolapse present?

A

A feeling of “something coming down” in the vagina
A dragging or heavy sensation in the pelvis

Urinary symptoms, such as incontinence, urgency, frequency, weak stream and retention

Bowel symptoms, such as constipation, incontinence and urgency

Sexual dysfunction, such as pain, altered sensation and reduced enjoyment

Women may have identified a lump or mass in the vagina, and often will already be pushing it back up themselves.

They may notice the prolapse will become worse on straining or bearing down.

203
Q

Examination: pelvic organ prolapse

A

Ideally, the patient should empty their bladder and bowel before examination of a prolapse.

When examining for pelvic organ prolapse, various positions may be attempted, including the dorsal and left lateral position.

A Sim’s speculum is a U-shaped, single-bladed speculum that can be used to support the anterior or posterior vaginal wall while the other vaginal walls are examined.

It is held on the anterior wall to examine for a rectocele, and the posterior wall for a cystocele.

The women can be asked to cough or “bear down” to assess the full descent of the prolapse.

204
Q

POP-Q grades

A

Grade 0: Normal
Grade 1: The lowest part is more than 1cm above the introitus
Grade 2: The lowest part is within 1cm of the introitus (above or below)
Grade 3: The lowest part is more than 1cm below the introitus, but not fully descended
Grade 4: Full descent with eversion of the vagina

205
Q

How can the severity of uterine prolapse be graded?

A

The severity of a uterine prolapse can be graded using the pelvic organ prolapse quantification (POP-Q) system

206
Q

What is uterine procidentia

A

A prolapse extending beyond the introitus can be referred to as uterine procidentia.

207
Q

Management of vaginal prolapse?

A

Conservative management

Vaginal pessary

Surgery

208
Q

Conservative management of pelvic organ proplapse is appropriate for women that are able to cope with mild symptoms, do not tolerate pessaries or are not suitable for surgery. What does it involve?

A

Physiotherapy (pelvic floor exercises)
Weight loss
Lifestyle changes for associated stress incontinence, such as reduced caffeine intake and incontinence pads
Treatment of related symptoms, such as treating stress incontinence with anticholinergic mediations
Vaginal oestrogen cream

209
Q

What is a vaginal pessary?

A

Vaginal pessaries are inserted into the vagina to provide extra support to the pelvic organs. They can create a significant improvement in symptoms and can easily be removed and replaced if they cause any problems.

210
Q

What should women using vaginal pessaries be advised?

A

Women often have to try a few types of pessary before finding the correct comfort and symptom relief.

Pessaries should be removed and cleaned or changed periodically (e.g. every four months). They can cause vaginal irritation and erosion over time.

Oestrogen cream helps protect the vaginal walls from irritation.

211
Q

Types of vaginal pessaries?

A

Ring pessaries are a ring shape, and sit around the cervix holding the uterus up

Shelf and Gellhorn pessaries consist of a flat disc with a stem, that sits below the uterus with the stem pointing downwards

Cube pessaries are a cube shape

Donut pessaries consist of a thick ring, similar to a doughnut

Hodge pessaries are almost rectangular. One side is hooked around the posterior aspect of the cervix and the other extends into the vagina.

212
Q

Potential complications of pelvic organ prolapse?

A

Pain, bleeding, infection, DVT and risk of anaesthetic

Damage to the bladder or bowel

Recurrence of the prolapse

Altered experience of sex

213
Q

Mesh repairs have been the subject of a lot of controversy over recent years. Mesh repairs involve inserting a plastic mesh to support the pelvic organs. After review, NICE recommend that mesh procedures should be avoided entirely. What complications might they cause?

A

Chronic pain

Altered sensation

Dyspareunia (painful sex) for the women or her partner

Abnormal bleeding

Urinary or bowel problems

Women presenting with possible complications of mesh repair should be referred to a specialist for assessment and management.

214
Q

What is urge incontinence?

A

Urge incontinence is caused by overactivity of the detrusor muscle of the bladder. Urge incontinence is also known as overactive bladder. The typical description is of suddenly feeling the urge to pass urine, having to rush to the bathroom and not arriving before urination occurs. Women with urge incontinence are very conscious about always having access to a toilet, and may avoid activities or places where they may not have easy access. This can have a significant impact on their quality of life, and stop them doing work and leisure activities.

215
Q

What is stress incontinence?

A

The pelvic floor consists of a sling of muscles that support the contents of the pelvic. There are three canals through the centre of the female pelvic floor: the urethral, vaginal and rectal canals. When the muscles of the pelvic floor are weak, the canals become lax, and the organs are poorly supported within the pelvis.

Stress incontinence is due to weakness of the pelvic floor and sphincter muscles. This allows urine to leak at times of increased pressure on the bladder. The typical description of stress incontinence is urinary leakage when laughing, coughing or surprised.

216
Q

What is mixed incontinence?

A

Mixed incontinence refers to a combination of urge incontinence and stress incontinence. It is crucial to identify which of the two is having the more significant impact and address this first.

217
Q

What is overflow incontinence?

A

Overflow incontinence can occur when there is chronic urinary retention due to an obstruction to the outflow of urine. Chronic urinary retention results in an overflow of urine, and the incontinence occurs without the urge to pass urine. It can occur with anticholinergic medications, fibroids, pelvic tumours and neurological conditions such as multiple sclerosis, diabetic neuropathy and spinal cord injuries. Overflow incontinence is more common in men, and rare in women. Women with suspected overflow incontinence should be referred for urodynamic testing and specialist management.

218
Q

Risk factors for urinary incontience?

A

Increased age
Postmenopausal status
Increase BMI
Previous pregnancies and vaginal deliveries
Pelvic organ prolapse
Pelvic floor surgery
Neurological conditions, such as multiple sclerosis
Cognitive impairment and dementia

219
Q

What modifiable risk factors should you ask about when assessing urinary incontinence?

A

Caffeine consumption

Alcohol consumption

Medications

Body mass index (BMI)

220
Q

What can you ask a patient presenting with urinary incontinence about to try and asses the severity of symptoms?

A

Frequency of urination

Frequency of incontinence

Nighttime urination

Use of pads and changes of clothing

221
Q

Examination of a patient with urinary incontinence?

A

Examination should assess the pelvic tone and examine for:

Pelvic organ prolapse

Atrophic vaginitis

Urethral diverticulum

Pelvic masses

During the examination, ask the patient to cough and watch for leakage from the urethra.

The strength of the pelvic muscle contractions can be assessed during a bimanual examination by asking the woman to squeeze against the examining fingers.

222
Q

The strength of the pelvic muscle contractions can be assessed during a bimanual examination by asking the woman to squeeze against the examining fingers. How can it be graded?

A

By the modified Oxford system

223
Q

Modified oxford system

A

0: No contraction
1: Faint contraction
2: Weak contraction
3: Moderate contraction with some resistance
4: Good contraction with resistance
5: Strong contraction, a firm squeeze and drawing inwards

224
Q

How might you investigate urinary incontinence?

A

A bladder diary should be completed, tracking fluid intake and episodes of urination and incontinence over at least three days. There should be a mix of work and leisure days.

Urine dipstick testing should be performed to assess for infection, microscopic haematuria and other pathology.

Post-void residual bladder volume should be measured using a bladder scan to assess for incomplete emptying.

Urodynamic testing can be used to investigate patients with urge incontinence not responding to first-line medical treatments, difficulties urinating, urinary retention, previous surgery or an unclear diagnosis. It is not always required where the diagnosis is possible based on the history and examination.

225
Q

What are urodynamic tests and what do they involve?

A

Urodynamic tests are a way of objectively assessing the presence and severity of urinary symptoms. Patients need to stop taking any anticholinergic and bladder related medications around five days before the tests.

A thin catheter is inserted into the bladder, and another into the rectum. These two catheters can measure the pressures in the bladder and rectum for comparison. The bladder is filled with liquid, and various outcome measures are taken

226
Q

Outcomes and measure taken in urodynamic testing?

A

Cystometry measures the detrusor muscle contraction and pressure

Uroflowmetry measures the flow rate

Leak point pressure is the point at which the bladder pressure results in leakage of urine. The patient is asked to cough, move or jump when the bladder is filled to various capacities. This assesses for stress incontinence.

Post-void residual bladder volume tests for incomplete emptying of the bladder

Video urodynamic testing involves filling the bladder with contrast and taking xray images as the bladder is emptied. Theses are only performed where necessary and not a routine part of urodynamic testing.

227
Q

Management of stress incontieince

A

Avoiding caffeine, diuretics and overfilling of the bladder
Avoid excessive or restricted fluid intake
Weight loss (if appropriate)
Supervised pelvic floor exercises for at least three months before considering surgery
Surgery
Duloxetine is an SNRI antidepressant used second line where surgery is less preferred

228
Q

Pelvic floor exercises?

A

Pelvic floor exercises are used to strengthen the muscles of the pelvic floor. They increase the tone and improve the support for the bladder and bowel. Pelvic floor exercises should be supervised by an appropriate professional, such as a specialist nurse or physiotherapist. Women should aim for at least eight contractions, three times daily.

229
Q

Surgical management of stress incontinence

A

Tension-free vaginal tape (TVT) procedures involve a mesh sling looped under the urethra and up behind the pubic symphysis to the abdominal wall. This supports the urethra, reducing stress incontinence.

Autologous sling procedures work similarly to TVT procedures but a strip of fascia from the patient’s abdominal wall is used rather than tape

Colposuspension involves stitches connecting the anterior vaginal wall and the pubic symphysis, around the urethra, pulling the vaginal wall forwards and adding support to the urethra

Intramural urethral bulking involves injections around the urethra to reduce the diameter and add support

Where the stress incontinence is caused by a neurological disorder or other surgical methods have failed, specialist centres may offer an operation to create an artificial urinary sphincter. This involves a pump inserted into the labia that inflates and deflates a cuff around the urethra, allowing women to control their continence manually.

230
Q

Management of urge incontinence?

A

Bladder retraining (gradually increasing the time between voiding) for at least six weeks is first-line

Anticholinergic medication, for example, oxybutynin, tolterodine and solifenacin

Mirabegron is an alternative to anticholinergic medications

Invasive procedures where medical treatment fails

231
Q

Concerns re use of antichollinergics to manage urge incontinence

A

Anticholinergic medications need to be used carefully, as they have anticholinergic side effects. These include dry mouth, dry eyes, urinary retention, constipation and postural hypotension. Importantly they can also lead to a cognitive decline, memory problems and worsening of dementia, which can be very problematic in older, more frail patients.

232
Q

In what condition is micrabegron contraindicated and why?

A

Uncontrolled hypertension.

Blood pressure needs to be monitored regularly during treatment.

It works as a beta-3 agonist, stimulating the sympathetic nervous system, leading to raised blood pressure. This can lead to a hypertensive crisis and an increased risk of TIA and stroke.

233
Q

Invasive options for overactive bladder that has failed to respond to retraining and medical management include what?

A

Botulinum toxin type A injection into the bladder wall

Percutaneous sacral nerve stimulation involves implanting a device in the back that stimulates the sacral nerves

Augmentation cystoplasty involves using bowel tissue to enlarge the bladder

Urinary diversion involves redirecting urinary flow to a urostomy on the abdomen

234
Q

What is atrophic vaginitis?

A

Atrophic vaginitis refers to dryness and atrophy of the vaginal mucosa related to a lack of oestrogen. Atrophic vaginitis can also be referred to as genitourinary syndrome of menopause. It occurs in women entering the menopause.

235
Q

Why does menopause cause symptoms such as atrophic vaginitis, thrush and pelvic organ prolapse?

A

The epithelial lining of the vagina and urinary tract responds to oestrogen by becoming thicker, more elastic and producing secretions.

As women enter the menopause, oestrogen levels fall, resulting in the mucosa becoming thinner, less elastic and more dry. The tissue is more prone to inflammation.

There are also changes in the vaginal pH and microbial flora that can contribute to localised infections.

Oestrogen also helps maintain healthy connective tissue around the pelvic organs, and a lack of oestrogen can contribute to pelvic organ prolapse and stress incontinence.

236
Q

Symptoms of atrophic vaginitis?

A

Itching

Dryness

Dyspareunia (discomfort or pain during sex)

Bleeding due to localised inflammation

237
Q

In which patients should you consider atrophic vaginitis as a diagnosis?

A

Older women presenting with recurrent urinary tract infections, stress incontinence or pelvic organ prolapse.

Treatment with topical oestrogen where appropriate may improve the symptoms of these conditions.

It is worth asking about symptoms of vaginal dryness and discomfort, as women will often be reluctant to bring it up during a consultation. It is straightforward to treat and can make a big difference to their quality of life.

238
Q

What will be seen O/E in atrophic vaginitis?

A

Pale mucosa

Thin skin

Reduced skin folds

Erythema and inflammation

Dryness

Sparse pubic hair

239
Q

How can atrophic vaginitis be managed?

A

Vaginal lubricants can help symptoms of dryness. Examples include Sylk, Replens and YES.

Topical oestrogen can make a big difference in symptoms. Options include:

Estriol cream, applied using an applicator (syringe) at bedtime
Estriol pessaries, inserted at bedtime
Estradiol tablets (Vagifem), once daily
Estradiol ring (Estring), replaced every three months

240
Q

Contraindications for topical oestrogen

A

Topical oestrogen shares many contraindications with systemic HRT, such as breast cancer, angina and venous thromboembolism. It is unclear whether long term use of topical oestrogen increases the risk of endometrial hyperplasia and endometrial cancer.

Women should be monitored at least annually, with a view of stopping treatment whenever possible.

241
Q

Primary amenorrhoea, little or no axillary and pubic hair, elevated testosterone suggest what syndrome

A

Androgen insensitivity syndrome

242
Q

Following chickenpox exposure in a non-immune pregnant woman, varicella-zoster immunoglobulin (VZIG) is only effective up to how many days post-exposure

A

Following chickenpox exposure in a non-immune pregnant woman, varicella-zoster immunoglobulin (VZIG) is only effective up to 10 days post-exposure

243
Q

Secondary amenorrhoea: low-level gonadotrophins indicate what cause?

A

Hypothalamic

244
Q

What is Turner syndrome?

A

Turner syndrome, a condition that affects only females, results when one of the X chromosomes (sex chromosomes) is missing or partially missing. Turner syndrome can cause a variety of medical and developmental problems, including short height, failure of the ovaries to develop and heart defects

245
Q

Raised FSH/LH in primary amenorrhoea

A

Consider gonadal dysgenesis (e.g. Turner’s syndrome)

246
Q

What form of HRT does not increase risk of VTE?

A

Transdermal HRT

247
Q

First line management of menorrhagia

A

Menorrhagia - intrauterine system (Mirena) is first-line

248
Q

Gonadotrophin-releasing hormone agonists (GnRH agonists) may be used as second-line medical management in patients with endometriosis if a combination of non-steroidal anti-inflammatories and the combined oral contraceptive pill have not controlled their symptoms. How do they work to treat symptoms?

A

GnRH agonists lead to the down-regulation of GnRH receptors, thus reducing oestrogen (and androgen) production. This reduces the symptoms of endometriosis as oestrogen thickens the uterine lining.

249
Q

Diagnostic criteria for PCOS

A

PCOS should be diagnosed if 2/3 of the following criteria are present:

Infrequent or no ovulation (thus oligomenorrhoea is the correct answer in this scenario)

ROTTERDAM CRITERIA

Clinical or biochemical signs of hyperandrogenism or elevated levels of total or free testosterone (no mention of ‘low levels of oestrogen’)

Polycystic ovaries on ultrasonography or increased ovarian volume (over 10cm3)

250
Q

Signs of hyperandrogegism that might suggest PCOS

A

hirsutism,
alopecia,
acne vulgaris occurring after adolescence

251
Q

When can SSRIs be used to treat premensutal syndrome?

A

either continuously or during the luteal phase

252
Q

Causes of primary amenorrhoea

A

Constitutional delay i.e. a late bloomer, has secondary sexual characteristics

Anatomical i.e. mullerian agenesis (patient develops secondary sexual characteristics and has variable absence of female sexual organs)

Imperforate hymen (characterised by cyclical pain and the classic bluish bulging membrane on physical examination)

Transverse vaginal septae (characterised by cyclical pain and retrograde menstruation)

Turner syndrome (XO chromosome)

Testicular feminisation syndrome (XY genotype, no internal female organs)

Kallmann syndrome (failure to secrete GNRH)

253
Q

Causes of secondary amenorrhoea?

A

Pregnancy

Patient is using contraception

Menopause

Lactational amenorrhoea

Hypothalamic amenorrhoea (suppression of GnRH due to stress, excessive exercise, eating disorder)

Endocrinological (hyperthyroidism, polycystic ovary disease, Cushing’s syndrome, hyperprolactinaemia, hypopituitarism)

Premature ovarian failure (autoimmune, chemotherapy, radiation therapy)

Asherman’s syndrome (iatrogenic intrauterine adhesions/cervical stenosis)

254
Q

Useful tests to consider in patients presenting with amenorrhoea

A

Pregnancy test

FSH/LH (if FSH is >20 in a woman <40 may suggest premature ovarian failure, if both are low it suggests a hypothalamic cause)

Thyroid function tests

Prolactin

Pelvic USS

255
Q

Definition of primary amenorrhoea

A

Patient has never had a period and
Is aged 14 or older with no secondary sexual characteristics,

Or over 16 if secondary sexual characteristics are present.

256
Q

Definition of secondary amenorrhoea

A

the patient has had no periods for >6 months but has had periods in the past.

257
Q

Why does PMB occur in vaginal atrophy

A

Vaginal mucosa becomes drier and thinner. This can then bleed, especially when there is contact on the mucosa such as during intercourse, leading to symptoms such as post-coital bleeding and dyspareunia.

258
Q

If analgesia doesn’t help endometriosis then what should be tried?

A

The combined oral contraceptive pill or a progestogen should be tried

259
Q

Long term complications of PCOS?

A

Subfertility
Diabetes mellitus
Stroke & transient ischaemic attack
Coronary artery disease
Obstructive sleep apnoea
Endometrial cancer

260
Q

Rectovaginal exam revealing uterosacral nodularity and tenderness is suggestive of what

A

Endometriosis

261
Q

What is FGM?

A

Female genital mutilation (FGM) involves surgically changing the genitals of a female for non-medical reasons. FGM is a cultural practice that usually occurs in girls before puberty. It is a form of child abuse and a safeguarding issue.

262
Q

Laws surrounding FGM

A

Female genital mutilation is illegal as stated in the Female Genital Mutilation Act 2003, and there is a legal requirement for healthcare professionals to report cases of FGM to the police.

263
Q

In which countries if FGM common practice?

A

FGM is a common cultural practice in many African countries. Somalia has the highest levels of FGM in any country.

Other countries with high rates are Ethiopia, Sudan and Eritrea. It also occurs in Yemen, Kurdistan, Indonesia and various parts of South and Western Asia.

264
Q

What is Type 1 FGM

A

Removal of part or all of the clitoris.

265
Q

What is type 2 FGM

A

Removal of part or all of the clitoris and labia minora. The labia majora may also be removed

266
Q

What is type 3 FGM

A

Narrowing or closing the vaginal orifice (infibulation)

267
Q

What is type 4 FGM

A

All other unnecessary procedures to the female genitalia

268
Q

Identifying cases of FGM

A

It is important to recognise risk factors for FGM to identify and ideally prevent cases from occurring. Two key risk factors to bear in mind are coming from a community that practise FGM and having relatives affected by FGM.

There are scenarios where it is worth considering the risk of FGM:

Pregnant women with FGM with a possible female child
Siblings or daughters of women or girls affected by FGM
Extended trips with infants or children to areas where FGM is practised
Women that decline examination or cervical screening
New patients from communities that practise FGM
Women may also present with the complications of FGM.

269
Q

Immediate complications of FGM

A

Pain
Bleeding
Infection
Swelling
Urinary retention
Urethral damage and incontinence

270
Q

Long term complications of FGM

A

Vaginal infections, such as bacterial vaginosis
Pelvic infections
Urinary tract infections
Dysmenorrhea (painful menstruation)
Sexual dysfunction and dyspareunia (painful sex)
Infertility and pregnancy-related complications
Significant psychological issues and depression
Reduced engagement with healthcare and screening

271
Q

What should be done when a patient is discovered to have had FGM

A

It is essential to educate patients and relatives that FGM is illegal in the UK. Discuss the health consequences of FGM.

It is mandatory to report all cases of FGM in patients under 18 to the police.

Other services should also be contacted:

Social services and safeguarding
Paediatrics
Specialist gynaecology or FGM services
Counselling

In patients over 18, there needs to be careful consideration about whether to report cases to the police or social services.
The RCOG recommends using a risk assessment tool to tackle this issue which includes considering whether the patient has female relatives that may be at risk.

If the unborn child of a pregnant woman affected by FGM is considered to be at risk, a referral should be made.

272
Q

What is de-infibulation?

A

A de-infibulation surgical procedure may be performed by a specialist in FGM in cases of type 3 FGM. This aims to correct the narrowing or closure of the vaginal orifice, improve symptoms and try to restore normal function.

273
Q

What is re-infibulation?

A

Re-infibulation (re-closure of the vaginal orifice) could be requested after childbirth. Performing this procedure is illegal

274
Q

What is Meig’s syndrome?

A

The three features of Meig’s syndrome are:
a benign ovarian tumour
ascites
pleural effusion

It is a rare condition usually occurring in woman over the age of 40 years and the ovarian tumour is generally a fibroma. It is managed by the surgical removal of the tumour, however the ascites and pleural effusion may need to be drained first to allow symptomatic relief and improve pulmonary function before the anaesthetic. It has excellent prognosis due to the benign nature of the tumour.

275
Q

Why is FSH raised in menopausal patients

A

At menopause (and in premature ovarian failure), ovarian function ceases, leading to high levels of FSH due to the removal of the negative feedback mechanisms.

276
Q

Most common complication of myomectomy

A

Adhesions

277
Q

Ovarian cysts in premenopausal women?

A

Functional ovarian cysts related to the fluctuating hormones of the menstrual cycle, and are very common in premenopausal women.

The vast majority of ovarian cysts in premenopausal women are benign.

Cysts in postmenopausal women are more concerning for malignancy and need further investigation.

278
Q

What does a diagnosis of PCOS require at least two of

A

Anovulation
Hyperandrogenism
Polycystic ovaries on ultrasound

279
Q

Presentation of ovarian cysts?

A

Most ovarian cysts are asymptomatic. Cysts are often found incidentally on pelvic ultrasound scans.

Occasionally, ovarian cysts can cause vague symptoms of:

Pelvic pain
Bloating
Fullness in the abdomen
A palpable pelvic mass (particularly with very large cysts such as mucinous cystadenomas)
Ovarian cysts may present with acute pelvic pain if there is ovarian torsion, haemorrhage or rupture of the cyst.

280
Q

Follicular cysts

A

Type of functional cyst

Follicular cysts represent the developing follicle. When these fail to rupture and release the egg, the cyst can persist. Follicular cysts are the most common ovarian cyst, they are harmless and tend to disappear after a few menstrual cycles. Typically they have thin walls and no internal structures, giving a reassuring appearance on the ultrasound.

281
Q

Corpeus luteum cyst

A

Type of functional cysts
Corpus luteum cysts occur when the corpus luteum fails to break down and instead fills with fluid. They may cause pelvic discomfort, pain or delayed menstruation. They are often seen in early pregnancy.

282
Q

Non functional ovarian cysts

A

Serous Cystadenoma

Mucinous Cystadenoma

Endometrioma

Dermoid Cysts / Germ Cell Tumours

Sex Cord-Stromal Tumours

283
Q

What type of ovarian cyst might occur in endometriosis?

A

Endometrioma

These are lumps of endometrial tissue within the ovary, occurring in patients with endometriosis. They can cause pain and disrupt ovulation.

284
Q

Sex Cord-Stromal Tumours are rare forms of ovarian cysts that can be benign or mallignant , what are the common subtypes

A

Sertoli–Leydig cell tumours and granulosa cell tumours

285
Q

Detailed history and examination of ?ovarian cyst that may suggest mallignancy

A

Abdominal bloating
Reduce appetite
Early satiety
Weight loss
Urinary symptoms
Pain
Ascites
Lymphadenopathy

286
Q

Premenopausal women with a simple ovarian cyst less than what size on ultrasound do not need further investigations.

A

5cm

287
Q

Why do simple ovarian cysts below 5cm in premenopausal women not require further investigations?

A

Less than 5cm cysts will almost always resolve within three cycles. They do not require a follow-up scan.

288
Q

Management of simple ovarian cysts in premenopausal women between 5 and 7cm

A

5cm to 7cm: Require routine referral to gynaecology and yearly ultrasound monitoring.

289
Q

Mama having simple ovarian cysts in premenopausal women above 7cm

A

Consider an MRI scan or surgical evaluation as they can be difficult to characterise with ultrasound.

290
Q

Cysts in postmenopausal women generally require what?

A

Cysts in postmenopausal women generally require correlation with the CA125 result and referral to a gynaecologist.

When there is a raised CA125, this should be a two-week wait suspected cancer referral.

Simple cysts under 5cm with a normal CA125 may be monitored with an ultrasound every 4 – 6 months.

291
Q

In post menopausal women, simple cysts under 5cm with a normal CA125 may be monitored how?

A

with an ultrasound every 4 – 6 months.

292
Q

Persistent or enlarging ovarian cysts may require what management?

A

Persistent or enlarging cysts may require surgical intervention (usually with laparoscopy). Surgery may involve removing the cyst (ovarian cystectomy), possibly along with the affected ovary (oophorectomy).

293
Q

Complications of ovarian cysts

A

Consider complications when patients present with acute onset pain. The main complications are:

Torsion
Haemorrhage into the cyst
Rupture, with bleeding into the peritoneum

294
Q

What is ovarian torsion?

A

Ovarian torsion is a condition where the ovary twists in relation to the surrounding connective tissue, fallopian tube and blood supply (the adnexa)

295
Q

When does ovarian torsion usually occur

A

Ovarian torsion is usually due to an ovarian mass larger than 5cm, such as a cyst or a tumour. It is more likely to occur with benign tumours. It is also more likely to occur during pregnancy.

296
Q

Why might ovarian torsion occur in younger girls?

A

Ovarian torsion can also happen with normal ovaries in younger girls before menarche (the first period), when girls have longer infundibulopelvic ligaments that can twist more easily.

297
Q

Why is ovarian torsion an emergency?

A

Twisting of the adnexa and blood supply to the ovary leads to ischaemia. If the torsion persists, necrosis will occur, and the function of that ovary will be lost. Therefore, ovarian torsion is an emergency, where a delay in treatment can have significant consequences. Prompt diagnosis and management is essential.

298
Q

How does ovarian torsion present?

A

The main presenting feature is sudden onset severe unilateral pelvic pain. The pain is constant, gets progressively worse and is associated with nausea and vomiting.

The pain is not always severe, and ovarian torsion can take a milder and more prolonged course. Occasionally, the ovary can twist and untwist intermittently, causing pain that comes and goes.

On examination there will be localised tenderness. There may be a palpable mass in the pelvis, although the absence of a mass does not exclude the diagnosis.

299
Q

Diagnosis of ovarian torsion?

A

Pelvic ultrasound is the initial investigation of choice.

Transvaginal is ideal, but transabdominal can be used where transvaginal is not possible.

It may show “whirlpool sign”, free fluid in pelvis and oedema of the ovary.

Doppler studies may show a lack of blood flow.

The definitive diagnosis is made with laparoscopic surgery.

300
Q

Management of ovarian torsion?

A

Patients need emergency admission under gynaecology for urgent investigation and management. Depending on the duration and severity of the illness they require laparoscopic surgery to either:

Un-twist the ovary and fix it in place (detorsion)

Remove the affected ovary (oophorectomy)

The decision whether to save the ovary or remove it is made during the surgery, based on a visual inspection of the ovary. Laparotomy may be required where there is a large ovarian mass or malignancy is suspected.

301
Q

Potential complications of ovarian torsion?

A

A delay in treating ovarian torsion can result in loss of function of that ovary. The other ovary can usually compensate, so fertility is not typically affected. Where this is the only functioning ovary, loss of function leads to infertility and menopause.

Where a necrotic ovary is not removed, it may become infected, develop an abscess and lead to sepsis. Additionally it may rupture, resulting in peritonitis and adhesions.

302
Q

What are cervical ectropian?

A

Cervical ectropion can also be called cervical ectopy or cervical erosion. Cervical ectropion occurs when the columnar epithelium of the endocervix (the canal of the cervix) has extended out to the ectocervix (the outer area of the cervix). The lining of the endocervix becomes visible on examination of the cervix using a speculum. This lining has a different appearance to the normal endocervix.

303
Q

Why do cervical ectropian cause post coital bleeding

A

The cells of the endocervix (columnar epithelial cells) are more fragile and prone to trauma. They are more likely to bleed with sexual intercourse. This means cervical ectropion often presents with postcoital bleeding

304
Q

Why do younger age, pregnancy and the COCP increase the risk of cervical ectropian

A

Cervical ectropion is associated with higher oestrogen levels, and therefore, is more common in younger women, the combined contraceptive pill and pregnancy.

305
Q

How do cervical ectropian present?

A

Many cervical ectropion are asymptomatic, and they are found incidentally during speculum examination for other reasons, for example, smear tests.

Ectropion may present with increased vaginal discharge, vaginal bleeding or dyspareunia (pain during sex). Intercourse is a common cause of minor trauma to the ectropion, triggering episodes of postcoital bleeding.

Examination of the cervix will reveal a well-demarcated border between the redder, velvety columnar epithelium extending from the os (opening), and the pale pink squamous epithelium of the ectocervix. This border is the transformation zone.

306
Q

Management of cervical ectropion

A

Asymptomatic ectropion require no treatment. Ectropion will typically resolve as the patient gets older, stops the pill or is no longer pregnant. Having a cervical ectropion is not a contraindication to the combined contraceptive pill.

Problematic bleeding is an indication for the treatment of cervical ectropion. Treatment involves cauterisation of the ectropion using silver nitrate or cold coagulation during colposcopy.

307
Q

What is seen here

A

Cervical ectropian

308
Q

What is a bartholins abscess?

A

Cysts can become infected, forming a Bartholin’s abscess. A Bartholin’s abscess will be hot, tender, red and potentially draining pus.

309
Q

Swelling in bartholins cyst

A

The swelling is typically unilateral and forms a fluid-filled cyst between 1 – 4 cm.

310
Q

Where are the Bartholins glands

A

The Bartholin’s glands are a pair glands located either side of the posterior part of the vaginal introitus (the vaginal opening). They are usually pea-sized and not palpable. They produce mucus to help with vaginal lubrication.

311
Q

Management of a Bartholins Cyst

A

Bartholin’s cysts will usually resolve with simple treatment such as good hygiene, analgesia and warm compresses. Incision is generally avoided, as the cyst will often reoccur. A biopsy may be required if vulval malignancy needs to be excluded (particularly in women over 40 years).

312
Q

How are Bartholins cysts diagnosed?

A

History and examination

313
Q

How is a Bartholins abscess managed

A

A Bartholin’s abscess will require antibiotics. A swab of pus or fluid from the abscess can be taken to culture the infective organism and check the antibiotic sensitivities. E. coli is the most common cause. Send specific swabs for chlamydia and gonorrhoea.

Surgical interventions may be required to treat a Bartholin’s abscess. There are two options for surgical management:

Word catheter (Bartholin’s gland balloon) – requires local anaesthetic
Marsupialisation – requires general anaesthetic

314
Q

What is a word catheter?

A

Surgical management of a Bartholins abscess

A Word catheter is a small rubber tube with a balloon on the end.

The procedure may be performed by an appropriately experienced person in a treatment room, rather than a theatre.

Local anaesthetic is used to numb the area.

An incision is made, and any pus is drained from the abscess.

The Word catheter is inserted into the abscess space, and inflated up to 3 ml with saline. The balloon fills the space and keeps the catheter in place.

Fluid can drain around the catheter, preventing a cyst or abscess reoccurring.

The tissue heals around the catheter, leaving a permanent hole.

The catheter can be deflated and carefully removed at a later date, once epithelisation of the hole has occurred.

315
Q

What is Marsupialisation

A

Surgical management of Bartholins abscess

Marsupialisation involves a general anaesthetic in a surgical theatre. An incision is made, and the abscess is drained. The sides of the abscess are sutured open. Suturing the abscess open allows continuous drainage of the area and prevents recurrence of the cyst or abscess.

316
Q

What is lichen sclerosis

A

Lichen sclerosus is a chronic inflammatory skin condition that presents with patches of shiny, “porcelain-white” skin. It commonly affects the labia, perineum and perianal skin in women. It can affect other areas, such as the axilla and thighs. It can also affect men, typically on the foreskin and glans of the penis.

317
Q

What is lichen sclerosis associated with (aetiology related)

A

Lichen sclerosus is thought to be an autoimmune condition. It is associated with other autoimmune diseases, such as type 1 diabetes, alopecia, hypothyroid and vitiligo.

318
Q

How is lichen sclerosis diagnosed?

A

The diagnosis of lichen sclerosus is usually made clinically, based on the history and examination findings. Where there is doubt, a vulval biopsy can confirm the diagnosis.

319
Q

Presentation of lichen sclerosis

A

The typical presentation in your exams is a woman aged 45 – 60 years complaining of vulval itching and skin changes in the vulva. The condition may be asymptomatic, or present with several symptoms:

Itching
Soreness and pain possibly worse at night
Skin tightness
Painful sex (superficial dyspareunia)
Erosions
Fissures
The Koebner phenomenon refers to when the signs and symptoms are made worse by friction to the skin. This occurs with lichen sclerosus. It can be made worse by tight underwear that rubs the skin, urinary incontinence and scratching.

320
Q

Appearance of lichen sclerosus?

A

Changes affect the labia, perianal and perineal skin. There can be associated fissures, cracks, erosions or haemorrhages under the skin. The affected skin appears:

“Porcelain-white” in colour
Shiny
Tight
Thin
Slightly raised
There may be papules or plaques

321
Q

Management of lichen sclerosis

A

Lichen sclerosis cannot be cured, but the symptoms can be effectively controlled. Lichen sclerosus is usually managed and followed up every 3 – 6 months by an experienced gynaecologist or dermatologist.

Potent topical steroids are the mainstay of treatment. The typical choice is clobetasol propionate 0.05% (dermovate). Steroids are used long term to control the symptoms of the condition. They also seem to reduce the risk of malignancy.

Steroids are initially used once a day for four weeks, then gradually reduced in frequency every four weeks to alternate days, then twice weekly. When the condition flares patients can go back to using topical steroids daily until they achieve good control. A 30g tube should last at least three months.

Emollients should be used regularly, both with steroids initially and then as part of maintenance.

322
Q

Complication of lichen sclerosis

A

The critical complication to remember is a 5% risk of developing squamous cell carcinoma of the vulva.

Other complications include:

Pain and discomfort
Sexual dysfunction
Bleeding
Narrowing of the vaginal or urethral openings

323
Q

What is this

A

Bartholins abscess

324
Q

What is the treatment for vaginal vault prolapse

A

The treatment for vaginal vault prolapse is sacrocolpoplexy

325
Q

What are nabothian cysts

A

Nabothian cysts are fluid-filled cysts often seen on the surface of the cervix. They are also called nabothian follicles or mucinous retention cysts. They are usually up to 1cm in size, but rarely can be more extensive. They are harmless and unrelated to cervical cancer.

326
Q

How and when might a nabothian cyst occur

A

The columnar epithelium of the endocervix (the canal) produces cervical mucus.

When the squamous epithelium of the ectocervix slightly covers the mucus-secreting columnar epithelium, the mucus becomes trapped and forms a cyst.

This can happen after childbirth, minor trauma to the cervix or cervicitis secondary to infection.

327
Q

How do nabothian cysts typically present?

A

Nabothian cysts are often found incidentally on a speculum examination. They do not typically cause any symptoms. Rarely, when they are very large, they may cause a feeling of fullness in the pelvis.

328
Q

How do nabothian cysts appear

A

Nabothian cysts appear as smooth rounded bumps on the cervix, usually near to os (opening). They can range in size from 2mm to 30mm, and have a whitish or yellow appearance.

329
Q

What is seen here?

A

Nabothian cysts

330
Q

Nabothian cyst management?

A

Where the diagnosis is clear, women can be reassured, and no treatment is required. They do not cause any harm and often resolve spontaneously.

If the diagnosis is uncertain, women can be referred for colposcopy to examine in detail. Occasionally they may be excised or biopsied to exclude other pathology. Rarely they may be treated during colposcopy to relieve symptoms.

331
Q

What type of HRT does not increase the risk of coronary artery disease

A

There is no increased risk of coronary artery disease with oestrogen-only HRT (the risk may even be lower with HRT)

332
Q

Contraindications to HRT

A

Undiagnosed abnormal bleeding
Endometrial hyperplasia or cancer
Breast cancer
Uncontrolled hypertension
Venous thromboembolism
Liver disease
Active angina or myocardial infarction
Pregnancy

333
Q

Considerations/asssesment prior to starting HRT

A

Take a full history to ensure there are no contraindications
Take a family history to assess the risk of oestrogen dependent cancers (e.g. breast cancer) and VTE
Check the body mass index (BMI) and blood pressure
Ensure cervical and breast screening is up to date
Encourage lifestyle changes that are likely to improve symptoms and reduce risks

334
Q

Progestogens vs progesterone vs progestins

A

Progestogens refer to any chemicals that target and stimulate progesterone receptors
Progesterone is the hormone produced naturally in the body
Progestins are synthetic progestogens

335
Q

What types of progestogens are used in HRT

A

C19 progestogens are derived from testosterone, and are more “male” in their effects. Examples are norethisterone, levonorgestrel and desogestrel. These may be helpful for women with reduced libido.

C21 progestogens are derived from progesterone, and are more “female” in their effects. Examples are progesterone, dydrogesterone and medroxyprogesterone. These may be helpful for women with side effects such as depressed mood or acne.

336
Q

HRT regime for women without a uterus

A

Oestrogen-only pills, for example, Elleste Solo or Premarin
Oestrogen-only patches, for example, Evorel or Estradot

337
Q

HRT regimes of perimenopasual women with periods?

A

Cyclical combined tablets, for example, Elleste-Duet, Clinorette or Femoston

Cyclical combined patches, for example, Evorel Sequi or FemSeven Sequi

Mirena coil plus oestrogen-only pills, for example, Elleste Solo or Premarin

Mirena coil plus oestrogen-only patches, for example, Evorel or Estradot

338
Q

HRT regimes in perimenopasual women

A

Continuous combined tablets, for example, Elleste-Duet Conti, Kliofem or Femoston Conti
Continuous combined patches, for example, Evorel-Conti or FemSeven Conti
Mirena coil plus oestrogen-only pills, for example, Elleste Solo or Premarin
Mirena coil plus oestrogen-only patches, for example, Evorel or Estradot

339
Q

What is Tibolone and how can it be used as HRT

A

Tibolone is a synthetic steroid that stimulates oestrogen and progesterone receptors. It also weakly stimulates androgen receptors. The effects on androgen receptors mean tibolone can be helpful for patients with reduced libido.

Tibolone is used as a form of continuous combined HRT. Women need to be more than 12 months without a period (24 months if under 50 years). They would be expected not to have breakthrough bleeding. Tibolone can cause irregular bleeding, resulting in further investigations to exclude other causes.

340
Q

Testosterone use in HRT

A

Testosterone is a male sex hormone (androgen). It is naturally present in low levels in women. Menopause can be associated with reduced testosterone, resulting in low energy and reduced libido (sex drive). Treatment with testosterone is usually initiated and monitored by a specialist. It is given by transdermal application, applied as a gel or a cream to the skin.

341
Q

HRT management points

A

Follow up three months after initiating HRT to review symptom and side effects
Side effects often settle with time, so it is worth persisting for at least three months with each regime
It takes 3 – 6 months of treatment to gain the full effects
Problematic or irregular bleeding is an indication for referral to a specialist
Ensure the woman has appropriate contraception
Stop oestrogen-containing contraceptives or HRT 4 weeks before major surgery (NICE guidelines 2018 – NG89)
Consider other causes of symptoms where they persist despite HRT (e.g. thyroid, liver disease and diabetes)

342
Q

Oestrogenic side effects of HRT

A

Nausea and bloating
Breast swelling
Breast tenderness
Headaches
Leg cramps

343
Q

Prosteogenic side effects of HRT

A

Mood swings
Bloating
Fluid retention
Weight gain
Acne and greasy skin

344
Q

Managing HRT side effects

A

Where patients experience side effects, it is worth changing the type of HRT or the route of administration (switch between patches and pills).

Patients with progestogenic side effects may do better switching to an HRT with a different form of progesterone. For example, patients with acne and mood swings may do better with a dydrogesterone progesterone (e.g. Femoston). In contrast, patients with reduced libido may do better with a norethisterone progesterone (e.g. Elleste-Duet). Progestogenic side effects can be avoided altogether by using a Mirena coil for endometrial protection.

Unscheduled bleeding can occur in the first 3 – 6 months of HRT (in women with a uterus). If unscheduled bleeding continues, consider referral for investigations, particularly regarding endometrial cancer.

345
Q

Stopping HRT

A

There is no specific regime for stopping HRT. It can be reduced gradually or stopped abruptly, depending on the preference of the woman. This choice does not affect long term symptoms. Gradually reducing the HRT may be preferable to reduce the risk of symptoms recurring suddenly.

346
Q

Polycystic ovarian syndrome characteristics

A

multiple ovarian cysts,
infertility,
oligomenorrhea,
hyperandrogenism
insulin resistance

347
Q

Anovulation

A

Absence of ovulation

348
Q

Oligovulation

A

Irregular infrequent ovulation

349
Q

Amenorrhoea

A

Absence of menstrual periods

350
Q

Oligomenorrhoea

A

Irregular, infrequent menstural periods

351
Q

What is hirsutism and what does it suggest

A

Hirsutism refers to the growth of thick dark hair, often in a male pattern, for example, male pattern facial hair

Hyperandrogenism (pcos)

352
Q

Presentation of PCOS

A

Oligomenorrhoea or amenorrhoea
Infertility
Obesity (in about 70% of patients with PCOS)
Hirsutism
Acne
Hair loss in a male pattern

353
Q

Complications (/other features) of PCOS

A

Insulin resistance and diabetes
Acanthosis nigricans
Cardiovascular disease
Hypercholesterolaemia
Endometrial hyperplasia and cancer
Obstructive sleep apnoea
Depression and anxiety
Sexual problems

354
Q

What is Acanthosis nigricans and why might it be seen in PCOS

A

Acanthosis nigricans describes thickened, rough skin, typically found in the axilla and on the elbows. It has a velvety texture. It occurs with insulin resistance.

355
Q

Differentials for hirsutism

A

PCOS

Medications, such as phenytoin, ciclosporin, corticosteroids, testosterone and anabolic steroids
Ovarian or adrenal tumours that secrete androgens
Cushing’s syndrome
Congenital adrenal hyperplasia

356
Q

Insulin resistance in PCOS

A

Insulin resistance is a crucial part of PCOS.

When someone is resistant to insulin, their pancreas has to produce more insulin to get a response from the cells of the body.

Insulin promotes the release of androgens from the ovaries and adrenal glands.

Therefore, higher levels of insulin result in higher levels of androgens (such as testosterone).

Insulin also suppresses sex hormone-binding globulin (SHBG) production by the liver.

SHBG normally binds to androgens and suppresses their function.

Reduced SHBG further promotes hyperandrogenism in women with PCOS.

The high insulin levels contribute to halting the development of the follicles in the ovaries, leading to anovulation and multiple partially developed follicles (seen as polycystic ovaries on the scan).

357
Q

What bloods are used to investigate PCOS

A

Testosterone
Sex hormone-binding globulin
Luteinizing hormone
Follicle-stimulating hormone
Prolactin (may be mildly elevated in PCOS)
Thyroid-stimulating hormone

358
Q

What will hormonal blood tests show in PCOS

A

Raised luteinising hormone
Raised LH to FSH ratio (high LH compared with FSH)
Raised testosterone
Raised insulin
Normal or raised oestrogen levels

359
Q

LH:FSH in PCOS

A

Raised

360
Q

Pelvic USS in PCOS

A

Pelvic ultrasound is required when suspecting PCOS.

A transvaginal ultrasound is the gold standard for visualising the ovaries. The follicles may be arranged around the periphery of the ovary, giving a “string of pearls” appearance. The diagnostic criteria are either:

12 or more developing follicles in one ovary
Ovarian volume of more than 10cm3

361
Q

Screening for diabetes in PCOS

A

The screening test of choice for diabetes in patients with PCOS is a 2-hour 75g oral glucose tolerance test (OGTT). An OGTT is performed in the morning prior to having breakfast. It involves taking a baseline fasting plasma glucose, giving a 75g glucose drink and then measuring plasma glucose 2 hours later. It tests the ability of the body to cope with a carbohydrate meal. The results are:

Impaired fasting glucose – fasting glucose of 6.1 – 6.9 mmol/l (before the glucose drink)
Impaired glucose tolerance – plasma glucose at 2 hours of 7.8 – 11.1 mmol/l
Diabetes – plasma glucose at 2 hours above 11.1 mmol/l

362
Q

In women with PCOS, It is crucial to reduce the risks associated with obesity, type 2 diabetes, hypercholesterolaemia and cardiovascular disease. How can these risks be reduced ?

A

Weight loss
Low glycaemic index, calorie-controlled diet
Exercise
Smoking cessation
Antihypertensive medications where required
Statins where indicated (QRISK >10%)

363
Q

Patients with PCOS should be assessed and managed for the associated features and complications, such as what?

A

Endometrial hyperplasia and cancer
Infertility
Hirsutism
Acne
Obstructive sleep apnoea
Depression and anxiety

364
Q

Most effective lifestyle intervention in management of PCOS?

A

Weight loss is a significant part of the management of PCOS. Weight loss alone can result in ovulation and restore fertility and regular menstruation, improve insulin resistance, reduce hirsutism and reduce the risks of associated conditions.

365
Q

What drug might be used to aid weight loss in women with PCOS?

A

Orlistat may be used to help weight loss in women with a BMI above 30. Orlistat is a lipase inhibitor that stops the absorption of fat in the intestines

366
Q

What risk factors are present or more likely to be present that mean women with PCOS are at increased risk of endometrial cancer?

A

Obesity
Diabetes
Insulin resistance
Amenorrhoea

367
Q

Options for managing risk of endometrial hyperplasia in women with PCOS

A

Mirena coil for continuous endometrial protection
Inducing a withdrawal bleed at least every 3 – 4 months with either:
Cyclical progestogens (e.g. medroxyprogesterone acetate 10mg once a day for 14 days)
Combined oral contraceptive pill

368
Q

Pathophysiology of increased endometrial cancer risk in women with PCOS

A

Under normal circumstances, the corpus luteum releases progesterone after ovulation. Women with PCOS do not ovulate (or ovulate infrequently), and therefore do not produce sufficient progesterone.

They continue to produce oestrogen and do not experience regular menstruation. Consequently, the endometrial lining continues to proliferate under the influence of oestrogen, without regular shedding during menstruation. This is similar to giving unopposed oestrogen in women on hormone replacement therapy. It results in endometrial hyperplasia and a significant risk of endometrial cancer.

369
Q

Investigating for endometrial hyperplasia in PCOS

A

Women with extended gaps between periods (more than three months) or abnormal bleeding need to be investigated with a pelvic ultrasound to assess the endometrial thickness. Cyclical progestogens should be used to induce a period prior to the ultrasound scan. If the endometrial thickness is more than 10mm, they need to be referred for a biopsy to exclude endometrial hyperplasia or cancer.

370
Q

Infertility in PCOS

A

Weight loss is the initial step for improving fertility. Losing weight can restore regular ovulation.

A specialist may initiate other options where weight loss fails. These include:

Clomifene
Laparoscopic ovarian drilling
In vitro fertilisation (IVF)

Metformin and letrozole may also help restore ovulation under the guidance of a specialist; however, the evidence to support their use is not clear.

Ovarian drilling involves laparoscopic surgery. The surgeon punctures multiple holes in the ovaries using diathermy or laser therapy. This can improve the woman’s hormonal profile and result in regular ovulation and fertility.

371
Q

What screening do women with PCOS require if they become pregnant

A

Women that become pregnant require screening for gestational diabetes. Screening involves an oral glucose tolerance test, performed before pregnancy and at 24 – 28 weeks gestation.

372
Q

Managing hirsutism in PCOS

A

Weight loss may improve the symptoms of hirsutism. Women are likely to have already explored options for hair removal, such as waxing, shaving and plucking.

Co-cyprindiol (Dianette) is a combined oral contraceptive pill licensed for the treatment of hirsutism and acne. It has an anti-androgenic effect, works as a contraceptive and will also regulate periods. The downside is a significantly increased risk of venous thromboembolism. For this reason, co-cyprindiol is usually stopped after three months of use.

Topical eflornithine can be used to treat facial hirsutism. It usually takes 6 – 8 weeks to see a significant improvement. The hirsutism will return within two months of stopping eflornithine.

Other options that may be considered by a specialist experienced in treating hirsutism include:

Electrolysis
Laser hair removal
Spironolactone (mineralocorticoid antagonist with anti-androgen effects)
Finasteride (5α-reductase inhibitor that decreases testosterone production)
Flutamide (non-steroidal anti-androgen)
Cyproterone acetate (anti-androgen and progestin)

373
Q

Topical treatment for hirsutism

A

Topical eflornithine can be used to treat facial hirsutism. It usually takes 6 – 8 weeks to see a significant improvement. The hirsutism will return within two months of stopping eflornithine.

374
Q

What COCP can be used to manage hirsutism and acne and for how long can it be used

A

Co-cyprindiol (Dianette) is a combined oral contraceptive pill licensed for the treatment of hirsutism and acne. It has an anti-androgenic effect, works as a contraceptive and will also regulate periods. The downside is a significantly increased risk of venous thromboembolism. For this reason, co-cyprindiol is usually stopped after three months of use.

375
Q

What is Ashermans syndrome and when does it typically occur

A

Asherman’s syndrome is where adhesions (sometimes called synechiae) form within the uterus, following damage to the uterus.

Usually Asherman’s syndrome occurs after a pregnancy-related dilatation and curettage procedure, for example in the treatment of retained products of conception (removing placental tissue left behind after birth). It can also occur after uterine surgery (e.g. myomectomy) or several pelvic infection (e.g. endometritis).

376
Q

How can endometrial curettage lead to Ashermans syndrome?

A

Endometrial curettage (scraping) can damage the basal layer of the endometrium. This damaged tissue may heal abnormally, creating scar tissue (adhesions) connecting areas of the uterus that are generally not connected. There may be adhesions binding the uterine walls together, or within the endocervix, sealing it shut.

These adhesions form physical obstructions and distort the pelvic organs, resulting in menstruation abnormalities, infertility and recurrent miscarriages.

Adhesions may be found incidentally during hysteroscopy. Asymptomatic adhesions are not classified as Asherman’s syndrome.

377
Q

Presentation of Ashermans syndrome

A

Asherman’s syndrome typically presents following recent dilatation and curettage, uterine surgery or endometritis with:

Secondary amenorrhoea (absent periods)
Significantly lighter periods
Dysmenorrhoea (painful periods)
It may also present with infertility.

378
Q

How can Ashermans syndrome be diagnosed

A

Hysteroscopy is the gold standard investigation, and can involve dissection and treatment of the adhesions
Hysterosalpingography, where contrast is injected into the uterus and imaged with xrays
Sonohysterography, where the uterus is filled with fluid and a pelvic ultrasound is performed
MRI scan

379
Q

How is Ashermans syndrome managed?

A

Management is by dissecting the adhesions during hysteroscopy. Reoccurrence of the adhesions after treatment is common.

380
Q

What is a bicornuate uterus and what complications may be associated

A

A bicornuate uterus is where there are two “horns” to the uterus, giving the uterus a heart-shaped appearance. It can be diagnosed on a pelvic ultrasound scan. A bicornuate uterus may be associated with adverse pregnancy outcomes. However, successful pregnancies are generally expected. In most cases, no specific management is required.

Typical complications include:

Miscarriage
Premature birth
Malpresentation

381
Q

What is an imperforate hymen and how might it present

A

Imperforate hymen is where the hymen at the entrance of the vagina is fully formed, without an opening.

Imperforate hymen may be discovered when the girl starts to menstruate, and the menses are sealed in the vagina. This causes cyclical pelvic pain and cramping that would ordinarily be associated with menstruation, but without any vaginal bleeding.

382
Q

Diagnosis and management of an imperforate hymen

A

An imperforate hymen can be diagnosed during a clinical examination. Treatment is with surgical incision to create an opening in the hymen.

383
Q

Theoretical potential complication of untreated imperforate hymen

A

Theoretically, if an imperforate hymen is not treated retrograde menstruation could occur leading to endometriosis.

384
Q

What is a transverse vaginal septae and how might it present

A

Transverse vaginal septae is caused by an error in development, where a septum (wall) forms transversely across the vagina.
This septum can either be perforate (with a hole) or imperforate (completely sealed).

Where it is perforate, girls will still menstruate, but can have difficulty with intercourse or tampon use.

Where it is imperforate, it will present similarly to an imperforate hymen with cyclical pelvic symptoms without menstruation. Vaginal septae can lead to infertility and pregnancy-related complications.

385
Q

How is a transverse vaginal septae diagnosed and managed

A

Diagnosis is by examination, ultrasound or MRI. Treatment is with surgical correction. The main complications of surgery are vaginal stenosis and recurrence of the septae.

386
Q

What is vaginal hypoplasia and vaginal agenisis, and why might they occur? What other structural abnormalities are associated? How are they managed?

A

Vaginal hypoplasia refers to an abnormally small vagina.

Vaginal agenesis refers to an absent vagina.

These occur due to failure of the Mullerian ducts to properly develop, and may be associated with an absent uterus and cervix.

The ovaries are usually unaffected, leading to normal female sex hormones. The exception to this is with androgen insensitivity syndrome, where there are testes rather than ovaries.

Management may involve the use of a vaginal dilator over a prolonged period to create an adequate vaginal size. Alternatively, vaginal surgery may be necessary.

387
Q

What is androgen insensitivity syndrome, and why does it occur?

A

Androgen insensitivity syndrome is a condition where cells are unable to respond to androgen hormones due to a lack of androgen receptors.

It is an X-linked recessive genetic condition, caused by a mutation in the androgen receptor gene on the X chromosome.

Extra androgens are converted into oestrogen, resulting in female secondary sexual characteristics. It was previously known as testicular feminisation syndrome.

388
Q

Androgen sensitivity syndrome genetics and phenotype

A

It is an X-linked recessive genetic condition, caused by a mutation in the androgen receptor gene on the X chromosome.

Patients with androgen insensitivity syndrome are genetically male, with XY sex chromosome.

However, the absent response to testosterone and the conversion of additional androgens to oestrogen result in a female phenotype externally. Typical male sexual characteristics do not develop, and patients have normal female external genitalia and breast tissue.

389
Q

Although patients with androgen insensitivity syndrome appear female, how do their reproductive organs differ from males?

A

Typical male sexual characteristics do not develop, and patients have normal female external genitalia and breast tissue. (Absent response to testosterone causing conversion to oestrogen)

Patients have testes in the abdomen or inguinal canal, and absence of a uterus, upper vagina, cervix, fallopian tubes and ovaries.

The female internal organs do not develop because the testes produce anti-Müllerian hormone, which prevents males from developing an upper vagina, uterus, cervix and fallopian tubes.

390
Q

Features/presentation of androgen insensitivity syndrome

A

Androgen insensitivity syndrome often presents in infancy with inguinal hernias containing testes. Alternatively, it presents at puberty with primary amenorrhoea.

Female external characteristics such as breasts and appearance of female genitalia

The insensitivity to androgens also results in a lack of pubic hair, facial hair and male type muscle development.

Patients tend to be slightly taller than the female average.

391
Q

Hormonal blood tests in androgen insensitivity syndrome

A

Raised LH

Normal or raised FSH

Normal or raised testosterone levels (for a male)

Raised oestrogen levels (for a male)

392
Q

Patients with partial androgen insensitivity syndrome, where there the cells have a partial response to androgens, present more ambigiously than patients with complete androgen insensitivity syndrome - how?

A

micropenis or clitoromegaly, bifid scrotum, hypospadias and diminished male characteristics.

393
Q

Complications of androgen insentivity syndrome

A

Patients are infertile, and there is an increased risk of testicular cancer unless the testes are removed.

Inguinal hernia

Ammenrohea

394
Q

Management of androgen insensitivity syndrome?

A

Management is coordinated by a specialist MDT, involving paediatrics, gynaecology, urology, endocrinology and clinical psychology. Medical input involves:

Bilateral orchidectomy (removal of the testes) to avoid testicular tumours
Oestrogen therapy
Vaginal dilators or vaginal surgery can be used to create an adequate vaginal length

Generally, patients are raised as female, but this is sensitive and tailored to the individual. They are offered support and counselling to help them understand the condition and promote their psychological, social and sexual wellbeing.

395
Q

Lifestyle changes to manage PMS

A

Smoking cessation
Small meals regularly
Complex Carbohydrate rich foods
Exercise
Alchol reduction
Regular sleep
Sleep reduction

396
Q

What type of ovarian cyst is the most likely culprit in ovarian torsion

A

Dermoid cysts, due to their size and density (secondary to mucin, teeth etc..), are most likely to tort. They will normally have a long pedicle because of their weight and as a result will twist (normally anti-clockwise).

397
Q

In a patient with PID, what tests are necessary

A

f) A high vaginal swab for nucleic acid amplification test (NAAT) is vital. This is to test for gonorrhoea and chlamydia.

A high vaginal Amies swab for bacterial and fungal culture should be performed, as well as an endocervical culture for gonorrhoea (due to increasing rates of resistance to first line cephalosporin therapies).

398
Q

Low grade CIN on colposcopy

A

Area of white, Ill definied

399
Q

Management of acute Bartholins abscess

A

Marsupialisation of the acute Bartholin’s abscess combines the drainage required to treat the abscess, as well as maintaining the gland drainage and reducing risk of recurrence.

It would be appropriate to start antibiotics if the patient was systemically unwell.

400
Q

Laproscopic findings in endometriosis

A

Powder burn spots affecting the pelvic peritoneum

401
Q

A high voiding detrusor pressure with a low peak flow rate is indicative of what type of incontinence?

A

Overflow

A high voiding detrusor pressure with a low peak flow rate is indicative of bladder outlet obstruction

402
Q

What might pelvic fluid be seen in an ovarian torsion

A

Pelvic fluid is a common but non-specific finding that represents transudate from the ovarian capsule due to venous and lymphatic obstruction

403
Q

How does red degneration of the fibroid present and when does it usually occur

A

Uterine fibroids are sensitive to oestrogen and can therefore grow during pregnancy. If growth outstrips their blood supply, they can undergo red or ‘carneous’ degeneration. This usually presents with low-grade fever, pain and vomiting. The condition is usually managed conservatively with rest and analgesia and should resolve within 4-7 days.

404
Q

Common long term complications of vaginal hysterectomy with antero-posterior repair include what?

A

Enterocoele
Vaginal vault prolapse