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Test bank for Psychopharmacology 4th Edition by Jerry Meyer | 2025 version | ALL chapters | 100% Verified |

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Equip yourself with the ultimate study resource for Psychopharmacology with this comprehensive Testbank for the 4th Edition. Authored by Jerry Meyer, this trusted guide provides 100% verified questions and answers for all chapters, ensuring you're fully prepared for your exams. With this testbank, you'll have access to a vast array of questions that cover every aspect of Psychopharmacology, helping you to reinforce your understanding of complex concepts and build confidence in your abilities. The 2025 version is designed to reflect the latest developments in the field, ensuring you're up-to-date with the most current knowledge. **Key Features:** * 100% verified questions and answers for all chapters of the 4th Edition * Comprehensive coverage of Psychopharmacology concepts and principles * Ideal study resource for students, educators, and professionals in the field * Reflects the latest developments in Psychopharmacology, ensuring you're current with industry knowledge * Helps you identify areas for improvement and reinforce your understanding of key concepts **Why Choose This Testbank?** This Testbank is your go-to study companion for Psychopharmacology, offering a wealth of knowledge and insights to help you excel in your exams. With its comprehensive and up-to-date content, you can trust that you're getting the best possible preparation for your studies. Whether you're a student, educator, or professional in the field, this testbank is an invaluable resource that will help you achieve your goals.

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Voorbeeld van de inhoud

Chapter 1 – Principles of Pharmacology

,(From Psychopharmacology: Drugs, the Brain, and Behavior, 4th Edition by
Meyer & Quenzer)
Each question has:

 A clinical or research-oriented scenario
 Answer choices (A–D)
 ✅ Correct Answer clearly labeled
 Deep rationale for correct & incorrect options



Chapter 1 – Principles of Pharmacology: 28 Extra-Advanced MCQs



1.

A pharmaceutical company is developing a new antipsychotic medication.
During initial studies, they observe that increasing the dose beyond a certain
point no longer improves therapeutic effect but increases side effects. What
pharmacological principle does this illustrate?

A. First-pass metabolism
B. Dose-response curve plateau
C. Bioavailability limitation
D. Half-life extension

✅ Correct Answer: B
Rationale: The dose-response curve plateau represents the maximal efficacy
of a drug. Beyond this point, further increasing the dose does not increase
therapeutic effect but often increases adverse effects. This is a core concept
in pharmacodynamics.

 A: First-pass metabolism involves drug metabolism in the liver before
reaching systemic circulation.
 C: Bioavailability refers to the proportion of drug entering circulation,
not dose-effect limits.

,  D: Half-life relates to drug elimination, not efficacy limits.



2.

A drug is administered orally, but only 40% reaches systemic circulation due
to extensive metabolism in the liver before entering the bloodstream. This
phenomenon is known as:

A. Blood-brain barrier filtration
B. First-pass effect
C. Renal clearance
D. Bioequivalence failure

✅ Correct Answer: B
Rationale: The first-pass effect refers to the metabolism of a drug in the liver
after oral administration but before it reaches systemic circulation.

 A: The blood-brain barrier limits CNS entry, not systemic circulation.
 C: Renal clearance involves excretion, not metabolism before
absorption.
 D: Bioequivalence relates to generic vs. brand drug comparisons.



3.

A 72-year-old patient is prescribed a benzodiazepine with a long half-life.
Over time, the drug accumulates, causing excessive sedation. This is most
likely due to:

A. Increased blood-brain barrier permeability
B. Reduced renal clearance due to age
C. Enzyme induction leading to faster metabolism
D. Decreased volume of distribution

, ✅ Correct Answer: B
Rationale: Elderly patients often have decreased renal and hepatic clearance,
leading to drug accumulation, especially for drugs with long half-lives.

 A: The BBB doesn’t become more permeable with normal aging.
 C: Enzyme induction would reduce, not increase, accumulation.
 D: Volume of distribution reduction would not typically cause
accumulation in this way.



4.

A researcher wants to compare the bioavailability of two formulations of the
same antidepressant. Which pharmacokinetic parameter should they focus
on?

A. Peak plasma concentration (Cmax)
B. Half-life (t½)
C. Area under the plasma concentration-time curve (AUC)
D. Therapeutic index

✅ Correct Answer: C
Rationale: AUC directly measures drug exposure over time and is the gold
standard for comparing bioavailability between formulations.

 A: Cmax reflects the rate of absorption, not total absorption.
 B: Half-life describes elimination.
 D: Therapeutic index measures safety margin, not bioavailability.



5.

Which of the following administration routes bypasses the first-pass
metabolism completely?

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