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NSG 6005 PHARM WEEKS 1-3 QUIZ (FROM OPERATION FNP CLASS 11) BASED ON FINAL EXAM!!

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NSG 6005 PHARM WEEKS 1-3 QUIZ (FROM OPERATION FNP CLASS 11) BASED ON FINAL EXAM!!

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NSG 6005 PHARM
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NSG 6005 PHARM

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NSG 6005 PHARM WEEKS 1-3 QUIZ (FROM
OPERATION FNP CLASS 11) BASED ON FINAL
EXAM!!
1. Genetic polymorphisms account for differences in metabolism, including:

☐ A. Poor metabolizers, who lack a working enzyme

☐ B. Intermediate metabolizers, who have one working, wild-type allele and one
mutant allele

☐ C. Extensive metabolizers, with two normally functioning alleles

☑ D. All of the above



2. Up to 21% of Asians are ultra-rapid 2D6 metabolizers, leading to:

☐ A. A need to monitor drugs metabolized by 2D6 for toxicity

☑ B. Increased dosages needed of drugs metabolized by 2D6, such as the
selective serotonin reuptake inhibitors

☐ C. Decreased conversion of codeine to morphine by CYP 2D6

☐ D. The need for lowered dosages of drugs, such as beta blockers



3. Rifampin is a nonspecific CYP450 inducer that may:

☐ A. Lead to toxic levels of rifampin and must be monitored closely

☐ B. Cause toxic levels of drugs, such as oral contraceptives, when
coadministered

☑ C. Induce the metabolism of drugs, such as oral contraceptives, leading to
therapeutic failure

☐ D. Cause nonspecific changes in drug metabolism

,4. Inhibition of P-glycoprotein by a drug such as quinidine may lead to:

☐ A. Decreased therapeutic levels of quinidine

☐ B. Increased therapeutic levels of quinidine

☐ C. Decreased levels of a coadministered drug, such as digoxin, that requires P-
glycoprotein for absorption and elimination

☑ D. Increased levels of a coadministered drug, such as digoxin, that requires P-
glycoprotein for absorption and elimination



5. Warfarin resistance may be seen in patients with VCORC1 mutation, leading to:

☐ A. Toxic levels of warfarin building up

☑ B. Decreased response to warfarin

☐ C. Increased risk for significant drug interactions with warfarin

☐ D. Less risk of drug interactions with warfarin



6. Genetic testing for VCORC1 mutation to assess potential warfarin resistance is
required prior to prescribing warfarin.

☐ A. True

☑ B. False



7. Pharmacogenetic testing is required by the U.S. Food and Drug Administration
prior to prescribing:

☐ A. Erythromycin

☐ B. Digoxin

,☑ C. Cetuximab

☐ D. Rifampin



8. Carbamazepine has a Black Box Warning recommending testing for the HLA-
B*1502 allele in patients with Asian ancestry prior to starting therapy due to:

☐ A. Decreased effectiveness of carbamazepine in treating seizures

☐ B. Increased risk for drug interactions

☑ C. Increased risk for Stevens-Johnson syndrome

☐ D. Resistance to carbamazepine



9. A genetic variation in how the metabolite of the cancer drug irinotecan (SN-38)
is inactivated by the body may lead to:

☐ A. Decreased effectiveness of irinotecan

☑ B. Increased adverse drug reactions, such as neutropenia

☐ C. Delayed metabolism of irinotecan into SN-38

☐ D. Concerns of irinotecan being carcinogenic



10. Patients who have a poor metabolism phenotype will have:

☑ A. Slowed metabolism of a prodrug into an active drug, leading to
accumulation of prodrug

☐ B. Accumulation of inactive metabolites

☐ C. A need for increased dosages of medications

☐ D. Increased elimination of active drug

, 11. Ultra-rapid metabolizers of drugs may have:

☐ A. To have dosages adjusted downward to prevent drug accumulation

☑ B. Active drug rapidly metabolized into inactive metabolites, leading to
therapeutic failure

☐ C. Increased elimination of active, nonmetabolized drug

☐ D. Slowed metabolism of a prodrug, leading to accumulation



12. A provider may consider testing for CYP2D6 variants prior to starting
tamoxifen to:

☐ A. Ensure no increased adverse reactions to tamoxifen

☐ B. Identify potential drug-drug interactions

☑ C. Reduce the likelihood of therapeutic failure

☐ D. Identify poor metabolizers of tamoxifen



The most frequent type of drug-food interaction is food:



1. Causing increased therapeutic drug levels



2. Affecting the metabolism of the drug



3. Altering the volume of distribution of drugs



4. Affecting the gastrointestinal absorption of drugs

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