Pharmacology 2060A/B Lecture Notes - Lecture 6: Bioavailability, Pharmacotherapy, Therapeutic Drug Monitoring

Multiple Choice questions 2 points each

1. Creatinine clearance is a commonly used estimate of:

A)Glomerular filtration rate (mL/min)

B)Tubular secretion (mL/min)

C)Total renal blood flow (mL/min)

D)Renal reabsorption (cc/min)

E)Steady state muscle breakdown rate (mcg/min)

2. Which of the following is not a measure of exposure?

a) Peak concentration

b) Time of maximum concentration

c) Area under the concentration time curve

d) Concentration measured 2 hours after dose administration

3. A clinically impactful drug interaction based upon inhibition of cytochrome P450 is most likely when:

a)The drug is metabolized by multiple enzymes

b)The drug has a narrow therapeutic index

c)There is limited variation in interindividual enzyme activity in the involved enzyme

d)The drug is a substrate of P-glycoprotein

e)All of the above

2. Why are dose-response (or concentration-response) analyses recommended for drug approval by a regulatory agency?

a) To increase the potential for adverse reactions in clinical trials in order to fully characterize the safety profile

b) To prolong the length of time it takes for drug approval

c) To maximize the likelihood that optimal drug dose will be prescribed after approval

d) To reduce the costs of clinical trials

e) To explore all possible disease state indications at time of initial approval

5. Which of the following is true of inhaled delivery of an aerosolized drug suspension?

a)An ideal drug would have low first pass hepatic metabolism to maximize systemic absorption

b)In contrast to milled powders, drugs in suspension are dosed in partial pressures

c)Efficiency of drug delivery by multi-dose inhalers is highly dependent upon patient technique

d)Typical multi-dose inhalers produce a very homogenous particle size of drug

e)Nebulized delivery of drug by face mask is not appropriate for children, demented or obtunded patients

6. The apparent volume of distribution (Vd):

a)Does not represent an actual physiologic volume

b)Can never be higher than total body water volume

c)Can be determined using only the half life of a drug

d)Will be large in a drug that is highly bound to serum proteins

e)Is usually small in drugs that require a loading dose

7. Which of the following characteristics of a drug make it most amenable to removal by hemodialysis?

a)Large volume of distribution

b)Large molecular weight

c)Strong protein binding

d)Good water solubility

8. Which is the best predictor of need for dosage adjustment in hepatic disease?

Child Pugh score

Portal splanchnic pressure (as measured by peripheral heart rate)

Degree of fibrosis and shunt on ultrasound

Levels of liver function tests

There is no single marker of hepatic dysfunction

9. Fexofenadine is not metabolized but is a P-glycoprotein (Pgp) substrate. How does St. John’s Wort cause decreased serum fexofenadine levels?

Inhibition of gut Pgp

Induction of gut PgP

Induction of CNS Pgp

Inhibition of biliary Pgp

None of the above

10. Which of the following is the best measure of renal function?

a)age

b)random urine creatinine concentration

c)spot plasma creatinine concentration

d)estimated creatinine clearance (Cockroft Gault)

e)Child-Pugh

11. Which pharmacokinetic parameter is the best measure of total systematic drug exposure after an oral dose?

a)Cmax

b)Elimination half life

c)Absorption rate constant

d)Area under the curve

e)Clearance

12. Which of the following is a mechanism that would cause a drug to have zero order elimination in humans?

a)Ultra-metabolizer genotype

b)Enterohepatic recirculation

c)High serum protein binding

d)Saturation of the prime metabolic enzyme

e)Sustained release version of a drug

13. Phase II metabolic metabolism:

a)Involves the covalent binding of a polar side chain

B)Always follows phase 1 metabolism

c)Employs breaking of aromatic ring structures

d)Is not subject to pharmacogenetic variation

e)Occurs exclusively pre-systemically, in the gut lumen

14. Which is not a high profile FDA Initiative?

a)Orphan Disease Act

b)Childhood Vaccine Act

c)Rare Disease Act

d)Breakthrough Drug Designation

15 In explaining risk posed by pharmaceutical R&D, which is not a development risk:

a)Patient population

b)Clinical endpoint

c)Predictability of trials

d)Competitive advantage

16. The key pivotal trials undertaken as part of the IND are part of which phase of the clinical drug development process?

a)Phase I

b)Phase II

c)Phase III

d)Phase IV

17. Which is not an EU Regulatory Process

a)Centralized Procedure

b)Certificate of Pharmaceutical Product Procedure

c)De-Centralized Procedure

d)Mutual Recognition

18. The role of experimental medicine strategies is to

a)Explore disease and drug biology to support go/no go decisions

b)Generate and fully validate biomarkers for FDA approval

c)Primarily to co-develop diagnostic tests to be filed with the NDA (new drug application)

d)Harmonize FDA and EMA phase 1 requirements

e)Define the pharmacokinetics of exploratory drugs in healthy volunteers or selected patient populations

1.The drug LSD has a half-life of 2.5 hours in plasma. What is the rate constant in hr-1? Report to 2 decimals.

2.A drug has a half-life of 4 hours. What is the rate constant in units of min-1? Report to 2 significant figures.

3.The drug amphetamine (molecular weight of 135.2) is often supplied as the phosphate salt of the form B•H₃PO_{4 .} If the drug is supplied in tablets that contain 22 mg of the drug salt, what is the amount of the drug itself in 1 tablet(s) in mg? Round to the nearest whole number.

4.The drug amphetamine (molecular weight of 135.2) is often supplied as the phosphate salt of the form B•H₃PO_{4 .} The drug is supplied in tablets that contain 23 mg of the drug salt and the bioavailability of the drug is 57%. If a person takes 4 tablet(s), what is the effective dose in mg? Report your result to the nearest whole number.

5.The drug amphetamine (molecular weight of 135.2) is often supplied as the phosphate salt of the form B•H₃PO_{4 .} The drug is supplied in tablets that contain 16 mg of the drug salt and the bioavailability of the drug is 41%. If a person takes 2 tablet(s), what is Cp? Assume the volume of distribution is 4.2 L/kg and the person weighs 172lbs. Report in ppb and with 1 decimal place.

6. The LD50 of a given drug is listed as 250mg/kg. How much of this drug would correspond to a lethal dose for a person weighing 173lbs? Report the result in grams to zero decimal places.

7. A drug has a plasma half-life of 2.4 hours. If the peak plasma concentration of this drug is 38.1 μg/L, how much time will elapse before the plasma concentration reaches 10.0 μg/L? Report your result in hours with 1 decimal place.

8. Fentanyl is an opiate that is about 10x as potent as morphine for pain relief. A plasma concentration of 15-20μg/L is usually fatal. A person is found non-responsive with 13 fentanyl patches surrounding them. Each patch has 100μg total fentanyl. Frequently, the patches are scaped and the contents "smoked" to deliver the drug directly to the bloodstream. If this person did so (using all the patches), what would be the peak plasma concentration of fentanyl? Asume the volume of distribution is 4L/kg and the person weighs 140.0lbs. Report in μg/L with 2 significant figures.

9.Fentanyl is an opiate that is about 10x as potent as morphine for pain relief. A plasma concentration of 21.1μg/L is usually fatal. One method of ingestion is to scrape the contents of the patch into a spoon, heat it, and inhale the vaporized drug. If a patch is labeled as delivering 75μg/hr for 66 hours, how many patches would have to be used in this way to reach the fatal peak plasma concentration? Asume the volume of distribution is 4L/kg and the person weighs 140.0lbs. Report to one decimal.

10.A drug that is taken orally reaches peak plasma concentration in 3 minutes and has a half-life of 42 minutes. A person takes enough of the drug to reach a peak plasma concentration of 40.4 μg/L. How long after ingestion of the drug will the plasma concentration reach 37 μg/L? Report your results in minutes, rounded to the nearest minute.

11.Heroin has a plasma half-life of 17 minutes as it rapidly metabolizes 6-monoacetylmorphine and eventually to morphine. Assume some ingests heroin by injection leading to a peak plasma concentration of 124.6μg/L. What will be the plasma concentration of heroin in the same units 44 minutes after injection? Report to the nearest whole number.

12.A drug is supplied in tablets that contain 5.0mg of the drug per tablet. The bioavailablity of this drug is 45%, the plasma half-life is 35 minutes, and the volume of distribution is 3L/kg. The drug is rapidly absorbed and reaches peak plasma concentration 25 minutes after ingestion. If a person weighing 190lbs takes two tablets, what will be the plasma concentration 3 hour(s) after he/she took the tablets? Report your result in ppb to one decimal.

13. A drug is supplied in tablets that contain 5.0mg of the drug per tablet. The bioavailablity of this drug is 64%, the plasma half-life is 41 minutes, and the volume of distribution is 4 L/kg. The drug is rapidly absorbed and reaches peak plasma concentration 39 minutes after ingestion. If a person weighing 207 lbs takes two tablets, what will be the plasma concentration 3 hour(s) after he/she took the tablets? Report your result in ppb to 2 decimals.