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Veterinary Pharmacology Course Mastery Guide — 100 Q&A Practice Set

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Escrito en
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Veterinary Pharmacology Course Mastery Guide — 100 Q&A Practice Set

Institución
CVA[24] - Certified Veterinary Assistant
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CVA[24] - Certified Veterinary Assistant











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Institución
CVA[24] - Certified Veterinary Assistant
Grado
CVA[24] - Certified Veterinary Assistant

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Subido en
8 de diciembre de 2025
Número de páginas
63
Escrito en
2025/2026
Tipo
Examen
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Veterinary Pharmacology Course Mastery
Guide — 100 Q&A Practice Set

Section 1: Fundamentals & Pharmacokinetics (Q1-15)

1. What is the study of how drugs move through the body called?
A) Pharmacodynamics
B) Pharmacokinetics
C) Pharmacotherapeutics
D) Toxicology

2. Which of the following administration routes bypasses first-pass metabolism?
A) Oral
B) Intravenous
C) Rectal
D) Sublingual

3. The volume of distribution (Vd) is highest for drugs that distribute extensively into:
A) Plasma
B) Fatty tissues
C) Muscle
D) Bone

4. What does a high extraction ratio indicate about a drug’s metabolism?
A) It is poorly absorbed
B) It is highly metabolized by the liver on first pass
C) It is excreted unchanged by the kidneys
D) It has low bioavailability

5. Which species lacks the ability to glucuronidate certain drugs due to low UDP-
glucuronosyltransferase activity?
A) Dog
B) Cat
C) Horse
D) Cow

,6. What term describes the time required for drug concentration to decrease by 50%?
A) Therapeutic index
B) Half-life
C) Clearance
D) Steady state

7. Phase I metabolism typically involves:
A) Conjugation
B) Oxidation by cytochrome P450 enzymes
C) Glucuronidation
D) Acetylation

8. Bioavailability is calculated by comparing the AUC of an extravascular route to:
A) Intramuscular route
B) Subcutaneous route
C) Intravenous route
D) Oral route

9. Which law explains passive diffusion of drugs across membranes?
A) Michaelis-Menten
B) Fick’s Law
C) Henderson-Hasselbalch
D) Stokes’ Law

10. Enterohepatic recirculation can prolong a drug’s effect because it is:
A) Excreted in bile, reabsorbed in intestine
B) Trapped in renal tubules
C) Bound to plasma proteins
D) Metabolized in lungs

11. Weak acids are best absorbed in the:
A) Stomach (acidic environment)
B) Small intestine (alkaline)
C) Colon
D) Mouth

12. The minimum effective concentration (MEC) is part of which pharmacokinetic
parameter?
A) Volume of distribution
B) Therapeutic range

, C) Clearance
D) Loading dose

13. Which parameter is used to calculate a loading dose?
A) Clearance
B) Half-life
C) Volume of distribution
D) Bioavailability

14. What is steady state?
A) When drug absorption equals elimination
B) When the drug is fully distributed
C) When maximum effect is reached
D) When metabolism stops

15. Which of these factors does NOT affect drug distribution?
A) Plasma protein binding
B) Blood flow to tissues
C) Lipid solubility
D) Tablet disintegration time



Section 2: Pharmacodynamics & Drug Receptors (Q16-30)

16. What does pharmacodynamics study?
A) What the body does to the drug
B) What the drug does to the body
C) Drug movement
D) Drug formulation

17. An agonist:
A) Blocks receptors
B) Binds and produces a response
C) Decreases receptor sensitivity
D) Only binds to enzymes

18. The therapeutic index (TI) is calculated as:
A) ED50 / LD50
B) LD50 / ED50

, C) TD50 / ED50
D) ED95 / LD5

19. Which term describes a drug’s ability to produce a maximal response?
A) Potency
B) Efficacy
C) Affinity
D) Tolerance

20. Competitive antagonism can be overcome by:
A) Decreasing agonist dose
B) Increasing agonist concentration
C) Giving an inverse agonist
D) Blocking metabolism

21. Drug tolerance often results from:
A) Increased absorption
B) Receptor up-regulation
C) Receptor down-regulation
D) Faster excretion

22. The ED50 represents:
A) Lethal dose in 50% of animals
B) Effective dose in 50% of animals
C) Toxic dose in 50% of animals
D) Dose causing side effects in 50%

23. Spare receptors are present when:
A) Maximal response occurs without full receptor occupancy
B) No receptors are available
C) All receptors must be occupied for effect
D) Receptors are inactive

24. Which drug-receptor interaction is reversible and competitive?
A) Covalent binding
B) Ionic bonding
C) Hydrogen bonding
D) Allosteric modulation

25. A partial agonist:
A) Has high efficacy alone
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