Chemotherapy

Question 1

<p>What are treatment options for cancer?</p>

Answer 1

<p>Surgery</p>

<p>Radiotherapy</p>

<p>Chemotherapy</p>

<p>Targeted therapies</p>

<p>Immunotherapy</p>

Question 2

<p>What are the steps of the cell cycle?</p>

Answer 2

<p>G1 (gap 1, preparation for DNA replication)</p>

<p>R (restriction point, point in G1 where the cell becomes committed)</p>

<p>S (DNA replication)</p>

<p>G2 (preparation for mitosis)</p>

<p>M (mitosis, cell divsion)</p>

Question 3

<p>What happens during G1 (gap 1)?</p>

Answer 3

<p>Preparation for DNA replication</p>

Question 4

<p>What is R during the cell cycle?</p>

Answer 4

<p>Restriction point, where the cell become committed</p>

Question 5

<p>What happens during S?</p>

Answer 5

<p>DNA replication</p>

Question 6

<p>What happens during G2?</p>

Answer 6

<p>Preparation for mitosis</p>

Question 7

<p>What happens during M?</p>

Answer 7

<p>Mitosis, cell division</p>

Question 8

<p>What are things that make the cell cycle go around?</p>

Answer 8

<p>Growth factors</p>

<p>Oncogenes</p>

Question 9

<p>What makes the cell cycle stop?</p>

Answer 9

<p>Tumour suppresor genes</p>

Question 10

<p>What does chemo delivery do?</p>

Answer 10

<p>Reduces the amount of cells</p>

Question 11

<p>What happens if the interval between chemo delivery is to long?</p>

Answer 11

<p>The cells grow back</p>

Question 12

<p>How is systematic therapy delivered?</p>

Answer 12

<p>Oral or intravenous route</p>

<p>Regular cycles with timing dependent on the findings from pharmacokinetics (half life, excretion)</p>

<p>May need to delay treatment if toxicites develop</p>

Question 13

<p>What needs to happen to chemotherapy if toxicities develop?</p>

Answer 13

<p>It needs to be delayed</p>

Question 14

<p>What are methods of assessing drug therapy?</p>

Answer 14

<p>CT scan</p>

<p>PET scan</p>

<p>Clinical examination</p>

Question 15

<p>What may assessing drug activity help?</p>

Answer 15

<p>Overall survival (OS)</p>

<p>Progression-free survival (PFS)</p>

<p>Improved quality of life (QoL)</p>

Question 16

<p>What is progression free survival?</p>

Answer 16

<p>Length of time during and after treatment of a disease that a patient lives with the disease but it does not get any worse</p>

Question 17

<p>What is overall survival?</p>

Answer 17

<p>The length of time from either the diagnosis or the start of treatment for a disease that the patient is still alive</p>

Question 18

<p>What does an adjuvant do?</p>

Answer 18

<p>Improve survival</p>

Question 19

<p>What does a neoadjuvant do?</p>

Answer 19

<p>May improve survival through increasing operability</p>

Question 20

<p>What is adjuvant treatment?</p>

Answer 20

<p>Treatment given in addition to a primary treatment</p>

Question 21

<p>What is neoadjuvant chemotherapy?</p>

Answer 21

<p>Medicines administered before surgery for the treatment of cancer</p>

Question 22

<p>What are some different classes of cytotoxic agents?</p>

Answer 22

<p>Alkylating agents</p>

<p>Anti-metabolites</p>

<p>Mitotic inhibitors</p>

<p>Antibiotics</p>

<p>Other</p>

Question 23

<p>What are some sites of action for cytotoxic agents?</p>

Answer 23

<p>Anti-metabolites prevent RNA synthesis by binding to DNA</p>

<p>Alkylating agents cross link guanine nucleobases, directly attacking DNA</p>

<p>Intercalating agents wedge between bases along DNA to stop polymerase and other proteins from binding (preventing DNA transcription and DNA duplication)</p>

<p>Spindle poisons act on tubulin, which forms the microtubules that attach to chromosomes during mitosis</p>

Question 24

<p>What do alkylating agents do?</p>

Answer 24

<p>Attach to free guanines on seperated DNA strands, impairing DNA replication</p>

Question 25

<p>What does the alkyl group of an alkylating agent allow?</p>

Answer 25

<p>Covalent bonds with other molecules</p>

Question 26

<p>What is an example of an alkylating agent?</p>

Answer 26

<p>Cisplatin</p>

Question 27

<p>What are some mechanisms of resistance against alkylating agents?</p>

Answer 27

<p>Decreases entry or increases exit of agent in cell</p>

<p>Inactivation of agent in cell</p>

<p>Enhanced repair of DNA lesions produced by alkylation</p>

Question 28

<p>How do antimetabolites work?</p>

Answer 28

<p>Similar structure to essential metabolites required by cell prior to cell division</p>

<p>Can be incorporated into new nuclear material or bind with vital enzymes</p>

Question 29

<p>What are examples of antimetabolites?</p>

Answer 29

<p>Antagonise folic acid</p>

<p>Antagonis purine</p>

Question 30

<p>What are examples of spindle poisons?</p>

Answer 30

<p>Vinca alkaloids</p>

<p>Taxanes</p>

Question 31

<p>What do vinca alkaloids do?</p>

Answer 31

<p>Metaphase arrest agents, blocking microtubule formation and spindle formation</p>

Question 32

<p>What do taxanes do?</p>

Answer 32

<p>Promote spindles and freeze cells at that stage</p>

Question 33

<p>What are the 2 classes of antimiotic antibiotics?</p>

Answer 33

<p>Anthracyclines</p>

<p>Non-anathracyclines</p>

Question 34

<p>What do antimiotic antibiotics do?</p>

Answer 34

<p>Intercalate and inhibit DNA and RNA synthesis</p>

<p>Bind to membranes and increase permeability of ions</p>

<p>Free radicals disrupt DNA chain and prevent mitosis</p>

Question 35

<p>Where during the cell cycle do alkylating agents act?</p>

Answer 35

<p>All of the stages</p>

Question 36

<p>Where during the cell cycle do antibiotics act?</p>

Answer 36

<p>End of G1 through to the start of G2</p>

Question 37

<p>Where during the cell cycle do antimetabolites?</p>

Answer 37

<p>S</p>

Question 38

<p>Where during the cell cycle do metabolic inhibitors act?</p>

Answer 38

<p>During M</p>

Question 39

<p>What is the aim of combination therapy?</p>

Answer 39

<p>Increase efficacy</p>

Question 40

<p>What are the principles underlying combination therapy?</p>

Answer 40

<p>Different mechanisms of action</p>

<p>Dissimilar toxicity profile (such as both do not act with neurotoxicity)</p>

Question 41

<p>What does having different mechanisms of action during combination therapy allow?</p>

Answer 41

<p>Synergistic or at least additive</p>

<p>Reduce risk of developing resistance</p>

Question 42

<p>What are some possible side effects of chemotherapy?</p>

Answer 42

<p>Vomiting</p>

<p>Nausea</p>

<p>Alopecia (loss of hair)</p>

<p>Tiredness</p>

Question 43

<p>What does moderately emetogenic chemotherapy refer to?</p>

Answer 43

<p>Moderate incidences of nausea and vomiting</p>

Question 44

<p>What does highly emetogenic chemotherapy refer to?</p>

Answer 44

<p>High incidents of nausea and vomiting</p>

Question 45

<p>What is CINV?</p>

Answer 45

<p>Chemotherapy induced nausea and vomiting</p>

Question 46

<p>What is peripheral CINV?</p>

Answer 46

<p>Where drugs act on enterochromaffin cells in the gastric glands which release serotonin which acts on vagal afferent 5-HT₃ receptors</p>

Question 47

<p>Where do the gastric glands release during peripheral CINV?</p>

Answer 47

<p>Serotonin</p>

Question 48

<p>What does serotonin act on during peripheral CINV?</p>

Answer 48

<p>5-HT₃receptors</p>

Question 49

<p>What is central CINV?</p>

Answer 49

<p>Drugs act on brainstem NK₃receptors and cause CINV</p>

Question 50

<p>What are examples of hormonal drugs?</p>

Answer 50

<p>Anti-oestrogen for breast cancer</p>

<p>Gonadorelin analogue</p>

<p>Anti-adrogen for prostate cancer</p>

Question 51

<p>What is anti-oestrogen used for?</p>

Answer 51

<p>Breast cancer</p>

Question 52

<p>What is anti-adrogen used for?</p>

Answer 52

<p>Prostate cancer</p>

Question 53

<p>What are some things targeted drugs act against?</p>

Answer 53

<p>Epidermal growth factor receptor (EGFR)</p>

<p>Vascular endothelial growth receptor (VEGR)</p>

Question 54

<p>What receptors do T lymphocytes have?</p>

Answer 54

<p>Activation and inhibitory receptors</p>

Question 55

<p>How does immunotherapy work?</p>

Answer 55

<p>Cancer cells hide from the immune system by binding to the self receptor PD1, but drugs can inhibit this</p>