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Test Bank For Brody-s Human Pharmacology, 7th Edition Editors Lynn Wecker & Susan L. Ingram.

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This original document contains the complete test bank for Brody’s Human Pharmacology, 7th Edition, edited by Lynn Wecker and Susan L. Ingram. It features comprehensive exam-style questions covering pharmacokinetics, pharmacodynamics, drug mechanisms, therapeutic uses, adverse effects, and clinical applications across major drug classes. The material is ideal for reinforcing core pharmacology concepts and preparing for medical, nursing, and health sciences examinations.

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Institution
Brody\\\'s Human Pharmacology
Course
Brody\\\'s Human Pharmacology

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Test Bank For Brody's Human Pharmacology, 7th Edition
Editors : Lynn Wecker & Susan L. Ingram

,Chapter 1: Introduction to Pharmacology

Based on Brody’s Human Pharmacology, 7th Edition (Wecker & Ingram)
For: Medical, Pharmacy, Nursing & Allied Health Students



Multiple-Choice Questions (1–20)



1. Which branch of pharmacology studies what the body does to a drug?

A. Pharmacodynamics
B. Pharmacotherapeutics
C. Pharmacokinetics
D. Toxicodynamics

ANS: C

Rationale:
Pharmacokinetics describes absorption, distribution, metabolism, and excretion (ADME).

• A is incorrect: Pharmacodynamics = what the drug does to the body.

• B refers to therapeutic use.

• D focuses on toxic effects.



2. A drug with high first-pass metabolism is best administered:

A. Orally
B. Intravenously
C. Rectally (lower rectum)
D. Subcutaneously

ANS: B

Rationale:
IV administration bypasses first-pass hepatic metabolism.
Oral drugs undergo portal circulation → liver metabolism.
Rectal administration partially bypasses first-pass but not completely.

,3. The therapeutic index (TI) is defined as:

A. ED50/TD50
B. TD50/ED50
C. LD50/ED90
D. EC50/IC50

ANS: B

Rationale:
TI = TD50 / ED50.
Higher TI = safer drug.
ED50 = effective dose in 50%
TD50 = toxic dose in 50%.



4. A competitive antagonist shifts a dose-response curve:

A. Downward
B. Rightward
C. Leftward
D. Upward

ANS: B

Rationale:
Competitive antagonists increase EC50 (decrease potency) → rightward shift.
Max efficacy remains unchanged.



5. Bioavailability refers to:

A. Rate of absorption
B. Fraction reaching systemic circulation
C. Drug distribution
D. Protein binding

ANS: B



6. Phase I metabolism primarily involves:

, A. Conjugation
B. Oxidation, reduction, hydrolysis
C. Renal filtration
D. Acetylation only

ANS: B



7. Which factor increases free drug concentration?

A. Increased albumin
B. Decreased albumin
C. Increased protein binding
D. Decreased clearance

ANS: B

Rationale:
Less albumin → more unbound (active) drug.



8. Steady state is achieved after approximately:

A. 1 half-life
B. 2 half-lives
C. 4–5 half-lives
D. 10 half-lives

ANS: C



9. An enzyme inducer would:

A. Increase drug levels
B. Decrease metabolism
C. Increase metabolism
D. Block receptors

ANS: C



10. Zero-order kinetics means:

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Brody\\\'s Human Pharmacology

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