Case 14- Anticancer drugs

Question 1

Adjuvant chemotherapy

Answer 1

After theoretical surgical cure to increase the chance of cure, reduces the risk of relapse, killing any microscopic disease left behind.

Question 2

Neo-adjuvant chemotherapy

Answer 2

Before the surgery to improve operability and chances of cure i.e. to shrink the tumour prior to removal

Question 3

Palliative chemotherapy

Answer 3

Used for symptom control not cure, advanced cancer

Question 4

Difference between targeted and non-targeted chemotherapy

Answer 4

Chemotherapy can be broadly divided into targeted and non-targeted. Non-targeted chemotherapy agents block the stages of the cell cycle, inhibiting DNA replication and mitosis. Targeted chemotherapy can differentiate between cancerous and non-cancerous cells.

Question 5

Types of non-targeted anicancerous agents

Answer 5

Alkylating agents, Platinum agents, Antimetabolites, Anthracyclines, Anti-microtubule agents.

Question 6

Cancer- Alkylating agents

Answer 6

For example, Cyclophosphamide. Covalently bind to Alkyl groups in the nucleotide Guanine, induces crosslinking DNA. The inhibits DNA replication and transcription so the cell undergoes cell cycle arrest and apoptosis.

Question 7

Examples of Alkylating agents (cancer)

Answer 7

• Cyclophosphamide-leukaemias, lymphoma and solid tumours

* Chlorambucil-lymphoma and chronic leukaemias

Question 8

Cancer- Platinum agents

Answer 8

For example, Cisplatin. Most widely used chemotherapy drugs. They bind to the nucleotide Guanine causing cross linked DNA which inhibits DNA replication and transcription. The cell undergoes cell cycle arrest and apoptosis. Connected to the Platinum you have two highly reactive Chlorine groups which interact with other proteins responsible for replication. They cause DNA protein cross links, induces stress mechanisms within the cells and the cells undergo apoptosis.

Question 9

Examples of Platinum agents

Answer 9

• Carboplatin- ovarian and lung cancer

* Cisplatin- testicular, lung, cervical, bladder and head/neck cancer

Question 10

Cancer- Antimetabolites

Answer 10

For example Methotrexate. They interfere with the normal cell metabolism of nucleic acids. Methotrexate inhibits the production of Pyrimidines and Purines by inhibiting the enzyme DHFR. Decreases nucleotides inhibiting DNA replication

Question 11

Normal production of Purines and Pyrimidines

Answer 11

Dietary folate is converted to FH2 which is converted by DHFR (Dihydrofolate reductase) into FH4. This is then converted to Purines or can be converted to Pyrimidines by Thymidylate synthase.

Question 12

Example of antimetabolites

Answer 12

• Methotrexate-acute leukaemia, non-Hodgkin’s lymphoma and solid tumours
• 5-Fluorouracil- GI and breast cancer

Question 13

Anthracyclines

Answer 13

For example Doxorubicin. These are anti-tumour antibiotics.

1) Inhibits Tropoisomerase 2 (Its normal role is to induce double stranded breaks to relax and stabilise DNA replication). This will prevent DNA relaxation and DNA reannealing which will create multiple DNA double strand breaks.
2) It can indirectly inhibit Helicase by intercalating into DNA and stabilising it, preventing it from being separated.
3) Produce reactive oxygen species which induce DNA/cell damage and apoptosis.

Question 14

Examples of Anthracyclines

Answer 14

• Doxorubicin- leukaemia, lymphoma and breast cancer
• Epirubicin- breast cancer
• Idarubicin- haematological cancer

Question 15

Cancer- anti microtubule agents

Answer 15

Disrupts the microtubule spindle which is required for effective separation of the chromatids. Microtubules are also important for cell migration (prevent metastasis), however this will cause a range of side effects as it disrupts normal cell function. Can be separated into Vinca Alkaloids and Taxanes. Affects mitosis but not DNA replication

Question 16

Types of anti-microtubule agents

Answer 16

• Vinca alkaloids- for example Vinicristine, prevents tubulin assembly, cant assemble the mitotic spindle. Chromatids cant separate, they experience cell arrest during anaphase.
• Taxane- for example Doxetaxel (breast and lung cancer). Prevents tubulin disassembly so you cant contract the mitotic spindle. Experience cell cycle arrest at the M phase checkpoint in Anaphase and die.

Question 17

Signs and symptoms of the menopause

Answer 17

• Hot flushes / night sweats
• Menstrual irregularities- can be heavier bleeding which occurs more regularly
• Difficulty sleeping
• Reduced sex drive (libido)
• Recurrent urinary tract infections (UTIs), increased frequency of urination, urinating at night
• Poor memory and concentration
• Headaches
• Mood changes, such as low mood or anxiety
• Palpitations
• Joint stiffness, aches and pain- Osteoporosis is the progressive loss of bone mass which alters bone microarchitecture, greater susceptibility to breaks. Osteopenia causes thinning of the bones.
• Reduced muscle mass

Question 18

What causes the Menopause

Answer 18

Oestrogen withdrawal

Question 19

Menopause- what causes vaginal dryness, itching or discomfort during sex

Answer 19

Its caused by atrophy, inflammation and reduced collagen. Thinning of the mucosal layer and thickening of the stroma. Thins out the vagina, making it more delicate. Reduction in oestrogen causes a loss in lubrication. There can be a reduction in elasticity making movement difficult and can cause bleeding and itch.

Question 20

Average age of the menopause

Answer 20

52

Question 21

Menopause- Vasomotor symptoms

Answer 21

Vasomotor symptoms i.e. hot flushes can by triggered by alcohol/caffeine, exercise and environmental temp changes. Due to the effect of fluctuating oestrogen levels on the thermoregulatory centre. Change to blood flow, blood might shift to the skin causing a feeling of warmth and flushing. Dilation in small blood vessels.

Question 22

Diagnosing the Menopause

Answer 22

In women over 45 the diagnosis of menopause does not need additional lab tests. Its 12 months since last menstrual period when the women is not using hormonal contraception, diagnosed retrospectively. Usually a transitional stage with irregular cycle and vasomotor symptoms, this is the peri-menopause stage.

Question 23

How many menstrual cycles in a womens life

Answer 23

400-500

Question 24

How to measure a womens ovarian reserve

Answer 24

Using an ultrasound or measuring FSH and AMH, will indicate a womens fertility

Question 25

Premature menopause

Answer 25

Amenorrhoea in women <40

Question 26

Causes of Premature menopause

Answer 26

• Insidious (Premature Ovarian Insufficiency)- chromosomal abnormalities i.e. Turners syndrome, Fragile X, Autoimmune, infection (TB, malaria, mumps)
• Iatrogenic-surgical menopause, consequence of cancer treatment (chemotherapy, radiotherapy)

Question 27

Diagnosis and investigations into the premature menopause

Answer 27

• Diagnosis based on symptoms and menstrual irregularities
• Endocrine test for FSH / LH / oestradiol- should be 6 weeks
• Cause investigated with genetic screening, pelvic USS, infection screen i.e. mumps, thyroid function
• Led by specialist reproductive endocrinologist

Question 28

Treatment for the premature menopause

Answer 28

• HRT- replacement rather than in addition, wont be exposed to the side effects older women have with increased levels of hormones.
• Cardiovascular health
• Skeletal health
• Reproductive wishes

Question 29

Hormonal status- post menopause

Answer 29

• FSH levels continually increase as it tries to stimulate the ovary to release oestrogen
• As without folliculogenesis there is no increase in oestrogen.
• There is no feedback loop or inhibin so FSH levels remain high, as no follicles remain then FSH cannot induce folliculogenesis. LH levels no longer surge but they also increase
• High FSH, LH. Low Oestrogen.

Question 30

Complications of HRT

Answer 30

• IHD i.e. angina/MI
• CVD
• VTE
• Untreated hypertension
• History of breast cancer
• Untreated endometrial hyperplasia (pre-cursor to cancer)/endometrial cancer
• Undiagnosed vaginal bleeding

Question 31

Deciding to go on HRT

Answer 31

HRT increases cardiovascular disease risk and breast cancer. Someone with a lot of risk factors for these conditions or who has already had them, might decide not to go on HRT. The risk with HRT to background risk can be multiplicative not adative. Important to know individual risk

Question 32

General advice for the menopause

Answer 32

• Life-style= avoidance of triggers (alcohol, caffeine), healthy BMI, exercise (can reduce vasomotor symptoms)
• Natural remedies- vitamins, can contain phito-oestrogen
• Vaginal moisturisers and lubricants

Question 33

Benefits of HRT

Answer 33

• Symptom control- vasomotor, vaginal dryness
• Reduces risk of osteoporosis
• Improves muscle mass
• Menstrual cycle control

Question 34

What makes up HRT

Answer 34

Can either be Oestrogen, Progesterone or Testosterone

Question 35

Nuclear/genomic action of HRT

Answer 35

• Oestrogen can bind to either ERα or Erβ receptors on the cell membrane
• Oestrogen then diffuses into the cytoplasm
• Binds to receptor in cytoplasm
• Translocated to nucleus
• Alters gene transcription
• Creates new mRNA
• Translation of new proteins through gene transcription
• Proteins produced depend upon the tissue type

Question 36

How HRT affects the bones

Answer 36

In the bones oestrogen prevents bone reabsorption. In the Myocardium oestrogen reduces inflammation, in skeletal muscle it regenerates muscle fibres. Can also help with insulin resistance preventing diabetes.

Question 37

Risks of HRT

Answer 37

Breast cancer, heart disease, pulmonary embolism stroke

Question 38

When to use local or systemic HRT

Answer 38

If you only have Urogenital symptoms (vagina, bladder) then apply local oestrogen, if you have additional symptoms use systemic oestrogen.

Question 39

Systemic HRT

Answer 39

• Without uterus- use Oestrogen (typically oral)
• With Uterus- Oestrogen and Progesterone
Using Progesterone reduces the risk of endometrial hyperplasia

Question 40

Sequential and continuous HRT

Answer 40

Sequential HRT- continuous oestrogen, sequential progesterone. Causes a withdrawal bleed, like a period. Given for perimenopause. If you gave the continuous preparation it would cause irregular periods
Continuous HRT- continuous oestrogen and progesterone which means there is no bleed, given post menopause

Question 41

HRT- testosterone preparation

Answer 41

Helps improve libido, energy, mood and concentration. Can be prepared in a gel, patch or implant. Can be particularly beneficial in younger women.

Question 42

SERM

Answer 42

Selective oestrogen receptor modulator. Non- hormonal drugs that help to increase oestrogen in some tissues but not others, and so there can be used to prevent the osteoporosis risk. Used when HRT cannot be used

Question 43

Pharmacokinetics of HRT

Answer 43

• First line therapy is normally oral
• Easy and convenient
• First pass effect
• Has to pass through the liver, and so some of it is metabolised, and so a higher dose needs to be given if the liver is overactive
• Shouldn’t be given to people with liver disease or people taking enzyme inducing medication, as this will increase breakdown lowering the concentration.
• Contra-indications- Nausea, and other GI symptoms
• Patients with a history of VTE should not be given the oral preparation
• Fluctuations in the hormone levels
• Patch/Gel/Implant are considered if taking the medication orally isn’t working or advisable

Question 44

Types of HRT given

Answer 44

Can also be given in gel, patch or implant. The patch can be in any location except the breast. The implant can be subdermal or intrauterine.

Question 45

Side effects of HRT

Answer 45

Caused by oestrogen- Fluid retention, Nausea, Headaches, Breast tenderness and Leg cramps
Caused by Progesterone- Irregular bleeding, PMS, bloating and depression

Question 46

How to reduce side effects of HRT

Answer 46

• Breast symptoms - Reduce Dose
• GI symptoms - take with food, to alleviate the symptoms
• Change type of hormone, or the brand of the hormone
• Change route of administration

Question 47

How long should you take HRT for

Answer 47

For people who had a premature menopause they should HRT till they are 52. There is an increase risk of side effects with duration of use, because of the increase in background relative risk with age. This should be considered when deciding to stop HRT. Normally a gradual stop to prevent reflux symptoms (dose reduction).

Question 48

HRT alternatives

Answer 48

• Selective oestrogen receptor modulator (SERM)
• Selective serotonin reuptake inhibitors (SSRI’s)- i.e. venlafaxine
• Serotonin-norepinephrine reuptake inhibitors (SNRIs) i.e. paroxetine
• Antihypertensive (alpha agonist) i.e. clonidine
• Antiepileptic i.e. Gabapentin

Question 49

Menopause and contraception

Answer 49

If last menstrual period is before 50 take contraception for 2 more years. If its after 50 take it for 1 more year. Contraception can help with the symptoms of menopause. Thought the chance of pregnancy is small you can still get it

Question 50

Risk factors for a mother having a baby with a neural tube defect

Answer 50

• They have already had a baby with a neural tube defect
• They or their partner have a close relative born with a neural tube defect
• They have type 1 (insulin dependent) diabetes (not gestational diabetes)
• They are obese, or take certain anti-epileptic medications, especially those containing sodium valproate or valproic acid

Question 51

Why is chemotherapy given in cycles and combinations

Answer 51

Cycles- stops cancer cells from recovering and regrowing

Combinations- targeting multiple signalling pathways makes it less likely for resistance to develop.

Question 52

What causes the side effects in chemotherapy

Answer 52

It inhibits cell division in all rapidly dividing cells

1) Hair/skin- allopecia, rash
2) Mucosal linings- nausea, ulcers, constipation, diarrhoea
3) Gonadal function
4) Bone marrow- reduced erythrocytes, leukocytes and platelets

Question 53

Anticancer drugs- Hormone antagonists

Answer 53

Stops cancers that develop in hormone sensitive tissue. Their growth may be inhibited by estrogen, progesterone, androgen receptor antagonists that stop the production of hormones

Question 54

Tamoxifen

Answer 54

1) SERM – Selective Estrogen Receptor Modulator
2) Anti-proliferative in breast tissue
3) Used in breast cancer treatment and prevention
4) 75% of breast cancer are Estrogen Receptor (ER) Positive
5) Competitive inhibibitor of Estradiol binding to the Estrogen receptor, Tamoxifen binds to the ER to form a dimer

Question 55

Protein kinase inhibitors i.e. Imatnib

Answer 55

Inhibits an oncogenic protein kinase (BCR-ABL) which causes chronic myeloid lukaemia. This protein kinase is only found in cancer cells and promotes cell proliferation. Imatinib inhibits ATP binding of BCR-ABL oncoprotein, preventing phosphorylation and activation of downstream substrates.

Question 56

Protein kinase inhibitors i.e. Imatnib

Answer 56

Inhibits an oncogenic protein kinase (BCR-ABL) which causes chronic myeloid lukaemia. This protein kinase is only found in cancer cells and promotes cell proliferation. Imatinib inhibits ATP binding of BCR-ABL oncoprotein, preventing phosphorylation and activation of downstream substrates.

Question 57

Cancer treatment- Immunotherapy

Answer 57

Activates the bodies own immune system to recognise and kill cancer cells by removing immune checkpoint inhibitors.

Question 58

Pd-1 receptor antagonists (Pembrolizumab)

Answer 58

Immunotherapy- a group of checkpoint inhibitors for the treatment of multiple solid cancers