Pharm 25 - Quick & Easy

Question 1

-famide & -phamide

Answer 1

alkylating agents: nitrogen mustards

Question 2

-platin

Answer 2

alkylating agents: platinum analogs

Question 3

-tecan & -rubicin

Answer 3

topoisomerase enzyme inhibitors

Question 4

-taxel & -istine

Answer 4

antimicrotubules

Question 5

-abine & 5-FU

Answer 5

antimetabolites

Question 6

-mab

Answer 6

monoclonal antibodies

Question 7

-nib

Answer 7

tyrosine kinase inhibitors

Question 8

(nitrogen mustard class)
Mesna:
MOA
S/E

Answer 8

○ Binds up acrolein to prevent hemorrhagic cystitis

○ Ifosfamide: has a build-up of acrolein that causes:
§ Hematuria, dysuria, increased urinary frequency
□ Requires bladder treatment to remove clots and continuous bladder irrigation

Question 9

Nitrogen mustards MOA

Answer 9

prevents cell division by cross-linking DNA strands

Question 10

ADE of nitrogen mustards

Answer 10

○ Hemorrhagic cystitis
§ Due to build up of a toxic metabolite (acrolein)
§ Aggressive hydration (IV/PO) essential
§ Adjust for renal dose
□ Causes acute tubular necrosis
○ Alopecia
○ CNS toxic

Question 11

Mesna is dosed with…

Answer 11

○ Given with ifosfamide

§ Not given with cyclophosphamide

Question 12

Which is less toxic: cyclophosphamide or ifosfamide? (nitrogen mustards)

Answer 12

Cyclophosphamide: Less toxic, and thus does not require Mesna

Question 13

CNS effects of ifosfamide (nitrogen mustard)

Answer 13

See confusion, drowsiness, hallucinations, depressive psychosis, seizures

Question 14

cold sensitivity drug

Answer 14

Oxaliplatin

Question 15

MOA of platinum analogs

Answer 15

prevents cell division by cross-linking DNA strands

Question 16

Nephrotoxicity order for the platinum analogs: place the following in order of greatest toxicity to least

carboplatin, cisplatin, oxaliplatin

Answer 16

Cisplatin > Carboplatin > Oxaliplatin

Question 17

Peripheral neuropathy order for the platinum analogs: place the following in order of greatest neuropathy to least

carboplatin, cisplatin, oxaliplatin

Answer 17

Cisplatin & Oxaliplatin > Carboplatin

Question 18

Highest emetic drug of the platinum analogs

Answer 18

Cisplatin: has two phases of acute and delayed

Question 19

Myelosuppression of carboplatin

Answer 19

thrombocytopenia

Question 20

Myelosuppression of cisplatin

Answer 20

anemia

Question 21

Ototoxic drug of the platnium analogs

Answer 21

cisplatin

Question 22

common reaction of the platinum analogs

Answer 22

hypersensitive infusion reactions

Question 23

nephrotoxic effects of cisplatin

Answer 23

Na and Mg wasting –> must be given with fluids that have NaCl and Mg

Question 24

Odd ADE of oxaliplatin

Answer 24

Pharyngolaryngeal dysethesia - “tingling,”“burning,”“constriction,” or unpleasant sensation felt in the mouth

Question 25

MOA of topoisomerase enzyme inhibitors

Answer 25

Inhibit topoisomerases
○ Topoisomerases are used to catalyze the breaking and rejoining of DNA strands during replication to relieve the strain that is placed on the double helix during unwinding
○ Inhibiting this action allows the drug to stop the replication of the individual cancer cell and thus the subsequent growth of the cancer

Question 26

Irinotecan ADE

Answer 26

○ Severe diarrhea
§ Some patients have a mutated allele that causes an increased risk for neutropenia and life threatening diarrhea
§ Pre-medicate patients with atropine if develop acute diarrhea
§ Delayed diarrhea: treat with oral and IV hydration, electrolyte replacement
□ Use loperamide (antidiarrheal that is opioid based and acts on circular/longitudinal muscles of the intestines to slow peristalsis and inhibit fluid/electrolyte secretion to reduce fecal volume)

Question 27

Irinotecan acute cholinergic etiology

Answer 27

combated with atropine

Question 28

Doxorubicin major ADE

Answer 28

Severely cumulative and permanent cardiotoxicity

Administer with dexrazoxane as it’s cardioprotective

Question 29

Doxorubicin complications (not cardiotoxicity)

Answer 29

Extravasation risk - use dexrazoxane to limit free radical formation

Question 30

Dexrazoxane

Answer 30

○ Gives cardioprotective effects from the cardiotoxicity of antitumor agents
§ Inhibits free radical formation to limit cardiotoxicity
§ Potentially decreases anthracycline antitumor effects

Question 31

Antimicrotubule MOA

Answer 31

○ Prevents microtubule assembly or disassembly

○ Microtubules are used to pull chromosomes apart during anaphase of the mitotic cell cycle
§ When this is interrupted, the cell can no longer replicate –> inhibits cellular replication

Question 32

Vincristine ADE

Answer 32

Fatal if administered intrathecally

§ Neurotoxic
□ Sensory and motor
® Trigeminal neuralgia: jaw pain, pharyngeal pain
® Constipation due to autonomic dysfunction - bowel regimen
□ Peripheral neuropathy
® Tingling and numbness

Question 33

Docetaxel & Paclitaxel ADE

Answer 33

§ Infusion related hypersensitivity
□ Give famotidine or diphenhydramine, steroid like dexamethasone (drug that’s used to treat N/V in chemo after other agents have failed)

§ Neurotoxic: cumulative peripheral neuropathy
§ Myelosuppression - neutropenia and anemia
§ Cardiovascular - peripheral edema, flushing
§ Dose adjusted for hepatic dysfunction

Question 34

Antimetabolites: MOA

Answer 34

o Act as false metabolites and are incorporated into DNA and RNA ultimately inhibiting synthesis of DNA to stop cellular reproduction/growth
o Capecitabine, Cytarabine, and Fluorouracil (purine/pyrimidine analogues) incorporate directly into DNA and replace nucleotides in the helix to disrupt DNA replication

Question 35

capecitabine, cytarabine, fluorouracil toxicities

Answer 35

§ Myelosuppression (pancytopenia)
□ This can occur for 3-25 days
□ VERY LONG TIME to have myelosuppression
§ Neurotoxicity: peripheral neuropathy, visual disturbance, somnolence
§ Adjust for renal dysfunction
§ Skin rash

Question 36

Fluorouracil (5-FU)

Answer 36

® Bolus administration can cause myelosuppression
® Continuous infusion can occur for 24 hours to 7 days
◊ Leads to mucosal damage (mucositis and diarrhea)
◊ Palmar-plantar erythrodysesthesia
§ Patients can have a genetic defect that can cause an increase in toxicity with this drug (dihydropyridine dehydrogenase - DPD)

Question 37

Methotrexate (MXT)

Answer 37

o Works quite well
§ Also inhibits folate for the patient, so must supplement with Leucovorin to combat

§ Drug interactions
	□ NSAIDs
	□ PPIs (dose dependent)
§ Adjusted for renal dysfunction 
	□ MTX can crystallize in urine and cause renal tubular damage

Question 38

Leucovorin

Answer 38

○ A reduced form of folic acid

§ Added to methotrexate to reduce myelosuppression of methotrexate

Question 39

Leucovorin - chemotherapy rescue agent

Answer 39

§ Actively competes with and displaces Methotrexate
□ Restores active folate stores required for DNA/RNA synthesis
□ Given 24-36 hours after the start of the MTX infusion

Question 40

Leucovorin - chemotherapy modulating agent

Answer 40

§ Combined with fluorouracil to increase enzyme inhibition and cause DNA damage

Question 41

· Antitumor antibiotics: bleomycin MOA

Answer 41

binds to DNA and acts like an alkylating agent, produces DNA cross-linking, ultimately inhibiting DNA and RNA synthesis

Question 42

Bleomycin use and ADE

Answer 42

Use: prostate cancer
ADE:
○ Bleomycin: “Bleo-Lung” –> pulmonary fibrosis
○ Infusion reactions - fever and chills
○ Dermatologic - hyperpigmentation, alopecia, palmar-plantar erythrodysesthesia

Question 43

bortezomib MOA

Answer 43

o MOA: inhibits proteasome enzyme complexes which regulate intracellular protein homeostasis
○ In some cases, can lead to increased cell death due to disruption of neoplastic cell cycle required proteins

Question 44

Bortezomib toxicity

Answer 44

○ Peripheral neuropathy: IV and SubQ
§ Usually administered SubQ as less neurotoxic (this is the drug that was given SubQ by nurses as they didn’t know what they were doing)
○ May cause herpes reactivation and thus require antiviral prophylaxis during therapy

Question 45

lenalidomide: use and MOA

Answer 45

o Use: treats multiple myeloma
o MOA: changes interferons and interleukins of the immune system
○ Inhibits proinflammatory cytokines
○ Stimulates proliferation of T cells to enhance cell mediated immunity
○ Inhibits trophic signals to angiogenic factors in cells
○ Inhibits growth of myeloma cells by inducing cell cycle arrest and cell death

Question 46

lenalidomide: black box warning

Answer 46

§ Myelosuppression: thrombocytopenia, neutropenia
§ Arterial/venous thromboembolic events (with dexamethasone)
§ Severe birth defects, embryo-fetal death

Question 47

Monoclonal antibody ADE toxicities

Answer 47

○ Infusion related
§ Titrated and commonly see fever/chills, dyspnea, nausea, anaphylaxis, and rigors
○ Myelosuppression (cytotoxic conjugates)
○ Immune mediated - these types of drugs are created through the use of animal immune systems and thus when introduced into the human body, there are MANY immune responses that can happen (also HIGHLY patient dependent on the reaction)
§ Toxic epidermal necrolysis, enterocolitis, hepatitis, progressive multifocal leukoencephalopathy, mucocutaneous reactions

Question 48

Rituximab toxicities

Answer 48

§ Hepatitis B virus reactivation - screen patients for HBV infection
§ CLL patients - Pneumocystis jirovecii and antiherpetic viral prophylaxis
§ High lymphocyte count - high infusion reaction potential

Question 49

Trastuzumab toxicites

Answer 49

CHF: Cardiotoxicity: heart failure, arrhythmia, cardiomyopathy

These effects ARE reversible

Question 50

Cetuximab toxicites

Answer 50

§ Electrolyte abnormalities - hypomagnesemia
§ Dermatologic: acneiform rash, skin rash
□ Rash resolves with the end of treatment
□ Patients like this drug as they feel like they can see it working/know it’s working when they get a rash
□ Rash needs to be treated with corticosteroids, ABX, antihistamines, moisturizing creams/lotions
§ Infusion related reactions

Question 51

Bevacizumab toxicites

Answer 51

○ HTN, impaired wound healing, hemorrhage, proteinuria/nephrotic syndrome, thromboembolism

○ Starves the tumor of the nutrients it needs

Question 52

Pembrolizumab toxicites

Answer 52

§ Immune-mediated: colitis, dermatitis, endocrinopathies, nephritis, pneumonitis
□ Because of these, check things like renal function, TSH

Question 53

Tyrosine kinase inhibitors purpose

Answer 53

○ Shut off a signaling pathway in one of many different ways
○ Catalyze the transfer of a phosphate group from ATP to tyrosine residues in proteins
§ Can bind on the inside or outside of the cell
○ Regulates messenger activity
Important in cellular regulation of proliferation/differentiation, motility, function, survival

Question 54

Tyrosine kinase inhibitors advantages

Answer 54

○ Single compound targeting multiple kinases
○ Efficacy in multiple tumor types
○ Oral therapy - convenient, less complex therapy

Question 55

Tyrosine kinase inhibitors disadvantages

Answer 55

○ Potential for drug-drug interactions
○ Still have significant toxicities
○ Patient monitoring less frequently - maybe less adherence/follow-up
○ Resistance is developing

Question 56

Hand-Foot syndrome drugs

Answer 56

§ Fluorouracil (antimetabolite)
§ Bleomycin (antitumor ABX)
§ Sorafenib (tyrosine kinase inhibitors)

Question 57

Cardiotoxic drugs

Answer 57

§ Doxorubicin (irreversible) - topoisomerase enzyme inhibitor
§ Trastuzumab (reversible) - monoclonal antibody