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Test Bank For Rapid Review Pharmacology, 3rd Edition With STUDENT CONSULT Online Access Authors : Thomas L. Pazdernik & Laszlo Kerecsen

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Ace your pharmacology exams with the Test Bank for Rapid Review Pharmacology, 3rd Edition by Thomas L. Pazdernik and Laszlo Kerecsen. This powerful study companion is designed to help students quickly review and reinforce essential pharmacology concepts. Packed with high-yield practice questions, it covers key topics such as drug mechanisms, therapeutic uses, adverse effects, and clinical applications—making it perfect for fast, effective revision. Ideal for medical, pharmacy, and health science students, this test bank supports exam preparation and helps build confidence with real-world, exam-style questions. Perfect for: Medical and pharmacy students Quick pharmacology revision Exam and board preparation Strengthening clinical knowledge #Pharmacology #MedicalStudents #PharmacyStudents #RapidReview #ExamPrep #StudySmart #HealthcareEducation

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Institution
Pharmacology
Course
Pharmacology

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Test Bank For Rapid Review Pharmacology, 3rd Edition
With STUDENT CONSULT Online Access

Authors : Thomas L. Pazdernik & Laszlo Kerecsen

, Rapid Review Pharmacology, 3rd Edition

Chapter 1: Pharmacokinetics.




Q1.

A drug with high lipid solubility and low molecular weight is most likely to:

A. Be poorly absorbed orally
B. Cross cell membranes easily
C. Be rapidly excreted unchanged
D. Have low bioavailability
E. Be restricted to plasma

Answer: B

Explanation:

• Lipid-soluble, small molecules cross membranes via passive diffusion.

Mechanism: Passive diffusion down concentration gradient

Clinical Correlation: CNS drugs must be lipid-soluble to cross BBB

Why others are wrong:

• A: Opposite—lipid solubility ↑ absorption

• C: Lipophilic drugs require metabolism

• D: Bioavailability usually ↑

• E: Hydrophilic drugs stay in plasma



Q2.

First-pass metabolism primarily occurs in the:

A. Kidney
B. Lung
C. Liver

, D. Brain
E. Plasma

Answer: C

Explanation:

• Portal circulation delivers drugs to liver → metabolism before systemic circulation

Mechanism: Hepatic enzyme degradation (CYP450)

Clinical Correlation:

• Oral drugs like propranolol have ↓ bioavailability

Incorrect options:

• A/B/D/E: Not major first-pass sites



Q3.

Which parameter best reflects drug distribution?

A. Clearance
B. Volume of distribution
C. Half-life
D. Bioavailability
E. Absorption rate

Answer: B

Explanation:

• Vd = amount of drug in body / plasma concentration

Mechanism: Indicates tissue vs plasma distribution

Clinical Correlation:

• High Vd → tissue binding (e.g., digoxin)

Incorrect:

• A: elimination

• C: time to eliminate

, • D/E: absorption



Q4.

A drug bound to plasma proteins is:

A. Pharmacologically active
B. Rapidly excreted
C. Unable to cross membranes
D. Free to act on receptors
E. Rapidly metabolized

Answer: C

Explanation:

• Only free drug = active

Mechanism: Protein binding limits diffusion

Clinical Correlation:

• Hypoalbuminemia → ↑ free drug toxicity

Incorrect:

• A/D: only free drug works

• B/E: binding prolongs duration



Q5.

Which route avoids first-pass metabolism?

A. Oral
B. Rectal (upper)
C. Sublingual
D. Intraperitoneal
E. Enteral

Answer: C

Explanation:

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