gynae cancers

Question 1

Histology cervical cancer

Answer 1

squamous cell cancer (80%)
adenocarcinoma (20%)

Question 2

Biggest risk factor in developing cervical cancer?

Answer 2

HPV 16,18 & 33

Question 3

What virsuses cause genital warts

Answer 3

HPV 6 & 11

Question 4

How does HPV cause cervical cancer?

Answer 4

HPV 16 & 18 produces the oncogenes E6 and E7 genes respectively
E6 inhibits the p53 tumour suppressor gene
E7 inhibits RB suppressor gene

Question 5

screening pathway for cervical cancer

Answer 5

1. Test for high-risk human papillomavirus strains (hrHPV)
   If negative return to normal recall
2. If positive → cytology
   If cytology negative, retest hrHPV in 12 months
   If hrHPV is then negative return to recall, if hrHPV positive repeat again in 12 months
   If hrHPV is positive at 24 months, cytology is normal refer to colposcopy anway
3. If cytology positive → colposcopy

Question 6

If sample is inadequate HPV cervical screening, what do you do?

Answer 6

Retest in 3 months
If inadequate again –> colposcopy

Question 7

Normal recall for cervical screening

Answer 7

Age 25 years: first invitation.
Age 25-49 years: screening every 3 years.
Age 50-64 years: screening every 5 years.
Women 65 years of age or older if they have not had a cervical screening test since 50 years of age or a recent cervical cytology sample is abnormal.

Question 8

cervical screening and pregnancy

Answer 8

cervical screening in pregnancy is usually delayed until 3 months postpartum unless missed screening or previous abnormal smears.

Question 9

women with HIV and cervical screening

Answer 9

Cervical cytology at diagnosis.

Cervical cytology should then be offered annually for screening.

Question 10

What is the test of cure pathway for CIN?

Answer 10

Individuals who have been treated for CIN1, CIN2, or CIN3 should be invited 6 months after treatment for a test of cure repeat cervical sample in the community

Question 11

Management of cervical intraepitlealial neoplasia

Answer 11

Large loop excision of the transformation zone (LLETZ)

Question 12

Cervical cancer stage 1A

Answer 12

Confined to cervix, only visible by microscopy and less than 7 mm wide:
A1 = < 3 mm deep
A2 = 3-5 mm deep

Gold standard of treatment is hysterectomy +/- lymph node clearance
Nodal clearance for A2 tumours

For patients wanting to maintain fertility, a cone biopsy with negative margins can be performed

Radical trachelectomy is also an option for A2

Question 13

Cervical cancer stage 1B

Answer 13

Confined to cervix, clinically visible or larger than 7 mm wide:
B1 = < 4 cm diameter
B2 = > 4 cm diameter

Radiotherapy with concurrent chemotherapy is advised
Radiotherapy may either be bachytherapy or external beam radiotherapy
Cisplatin is the commonly used chemotherapeutic agent

For B2 tumours: radical hysterectomy with pelvic lymph node dissection

Question 14

Stage II and III cervical cancer

Answer 14

Stage 2: Extension of tumour beyond cervix but not to the pelvic wall
A = upper two thirds of vagina
B = parametrial involvement

Stage 3: Extension of tumour beyond the cervix and to the pelvic wall
A = lower third of vagina
B = pelvic side wall

NB: Any tumour causing hydronephrosis or a non-functioning kidney is considered stage III

Radiation with concurrent chemotherapy
Radiotherapy may either be bachytherapy or external beam radiotherapy
Cisplatin is the commonly used chemotherapeutic agent

If hydronephrosis, nephrostomy should be considered

Question 15

Stage IV cervical cancer

Answer 15

Extension of tumour beyond the pelvis or involvement of bladder or rectum
A = involvement of bladder or rectum
B = involvement of distant sites outside the pelvis

Radiation and/or chemotherapy is the treatment of choice
Palliative chemotherapy may be best option for stage IVB

Question 16

What complications is there with LLETZ and cone biopsy

Answer 16

pre term labour in future pregnancies

Question 17

What does FSH do?

Answer 17

development of follicle beyond secondary
stimulates granulosa cells to multiply and produce oestrogen
Induces LH receptors on granulosa cells of the dominant follicle

Question 18

What does oestrogen do?

Answer 18

stimulates proliferation of granulosa cells
exerts negative feedback on the secretion of gonadotrophins
works with progesterone to maintain lining in luteal phase

Question 19

What does LH do?

Answer 19

stimulates theca cells to synthesise androgens
the mid-cycle surge in LH causes ovulation

Question 20

What does progesterone do?

Answer 20

Helps to build and maintain endometrial lining
progesterone is produced in large amounts by the corpus luteum to maintain the lining

the drop in progesterone due to degeneration of corpus luteum (due to no hCG) causes endmetrial shedding

Question 21

what are the 4 key follicular stages

Answer 21

Primordial follicles
Primary follicles
Secondary follicles
Antral follicles (also known as Graafian follicles)

Question 22

Histology of most endometrail cancers

Answer 22

adenocarcinoma

Question 23

risk factors for endometrial cancer

Answer 23

obesity
Nulliparity (Nulliparity is a risk factor for endometrial cancer. This is because during pregnancy, the balance of hormones shifts towards progesterone, which is a protective factor.)
early menarche
late menopause
unopposed oestrogen. The addition of a progestogen to oestrogen reduces this risk (e.g. In HRT). The BNF states that the additional risk is eliminated if a progestogen is given continuously
diabetes mellitus
tamoxifen
polycystic ovarian syndrome
hereditary non-polyposis colorectal carcinoma

Question 24

2 week wait criteria for ?endometrial cancer

Answer 24

Age over 55 with post menopausal bleeding (must be >12 months since last period)

Consider if over 55 and:
Unexplained vaginal discharge
Visible haematuria plus raised platelets, anaemia or elevated glucose levels

Question 25

Investigations for endometrial cancer?

Answer 25

Transvaginal ultrasound for endometrial thickness (normal is less than 4mm post-menopause)

Hysteroscopy with endometrial biopsy

Pipelle biopsy, which is highly sensitive for endometrial cancer making it useful for excluding cancer

Question 26

Stages of endometrial cancer?

Answer 26

Stage 1: Confined to the uterus
Stage 2: Invades the cervix
Stage 3: Invades the ovaries, fallopian tubes, vagina or lymph nodes
Stage 4: Invades bladder, rectum or beyond the pelvis

Question 27

Managemnet of endometrial cancer

Answer 27

total abdominal hysterectomy with bilateral salpingo-oophorectomy, also known as a TAH and BSO (removal of uterus, cervix and adnexa).

progestogen therapy is sometimes used in frail elderly women not consider suitable for surgery

Question 28

how may endometrial hyperplasia present?

Answer 28

intermenstrual bleeding

Question 29

What is endometrial hyperplasia ?

types?

Answer 29

abnormal proliferation of the endometrium in excess of the normal proliferation that occurs during the menstrual cycle. A minority of patients with endometrial hyperplasia may develop endometrial cancer

types:
hyperprolifertaion without atypia
atypical hyperplasia

Question 30

Management of endometrial hyperplasia?

Answer 30

Intrauterine system (e.g. Mirena coil)
Continuous oral progestogens (e.g. medroxyprogesterone or levonorgestrel) and retest in 3 months

If atypia : hysterectomy advised

Question 31

Invetsigations for ovarian cancer?

Answer 31

CA-125

If CA-125 is over 35 the do abdo USS

Diagnosis is difficult and usually involves CT for staginh and diagnostic laparotomy

Question 32

Most common ovarian cancer histlogy

Answer 32

epithelial cell tumour - serous tumour

Question 33

What are teratomas?

Answer 33

germ cell tumours

Question 34

Particular complication with teratomas?

Answer 34

ovarian torison

Question 35

Blood tests in teratomas

Answer 35

raised alpha-fetoprotein (α-FP)
raised human chorionic gonadotrophin (hCG)

Question 36

Risk factors for ovarian cancer

Answer 36

Age (peaks age 60)
BRCA1 and BRCA2 genes (consider the family history)
Increased number of ovulations
Obesity
Smoking
Recurrent use of clomifene

Factors that increase the number of ovulations, increase the risk of ovarian cancer. These include:
Early-onset of periods
Late menopause
No pregnancies

Question 37

2 week wait criteria for ovarian cancer

Answer 37

Ascites
Pelvic mass (unless clearly due to fibroids)
Abdominal mass

Question 38

What investigation should women under 40 years with a complex ovarian mass have

Answer 38

?teratoma

Alpha-fetoprotein (α-FP)
Human chorionic gonadotropin (HCG)

Question 39

What can raise CA-125?

Answer 39

Endometriosis
Fibroids
Adenomyosis
Pelvic infection
Liver disease
Pregnancy

Question 40

Management ovarian cancer

Answer 40

Ovarian cancer will be managed by a specialist gynaecology oncology MDT. It usually involves a combination of surgery and chemotherapy.

Question 41

Management ovarian cancer

Answer 41

Ovarian cancer will be managed by a specialist gynaecology oncology MDT. It usually involves a combination of surgery and chemotherapy.

Question 42

Stages of ovarian cancer

Answer 42

Stage 1: Confined to the ovary
Stage 2: Spread past the ovary but inside the pelvis
Stage 3: Spread past the pelvis but inside the abdomen
Stage 4: Spread outside the abdomen (distant metastasis)

Question 43

Most common histology vulval cancer

Answer 43

squamous cell carcinomas

Question 44

Invetsigations for vulval cancer

Answer 44

Biopsy of the lesion
Sentinel node biopsy to demonstrate lymph node spread
Further imaging for staging (e.g. CT abdomen and pelvis)

Question 45

management of lichen sclerosus

Answer 45

topical steroids and emollients

Question 46

Presentation of vaginal cancer?

Answer 46

abnormal discharge

Question 47

management vulval cancer?

Answer 47

Wide local excision to remove the cancer
Groin lymph node dissection
Chemotherapy
Radiotherapy

Question 48

what do theca cells do?

Answer 48

stimulated by LH to make androgen which can be converted to oestrogen by granulosa cells

Question 49

what do granulosa cells do?

Answer 49

stimulated by FSH to produce estrodiol