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NUR 600 Exam 1 – Advanced Clinical Pharmacology – (2026) Actual Questions & Answers (STU)

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NUR 600 Exam 1 – Advanced Clinical Pharmacology is a focused exam prep PDF designed for St. Thomas University nursing students preparing for Exam 1. This resource includes exam-style questions that mirror the actual exam and help students review high-priority Advanced Clinical Pharmacology concepts in a clear, organized format. The guide supports preparation for multiple-choice questions, clinical scenarios, and case-based pharmacology questions. It is useful for reinforcing medication safety, drug classifications, pharmacokinetics, pharmacodynamics, patient-centered prescribing, adverse effects, nursing implications, and advanced clinical decision-making. With a printable and tablet-friendly format, students can study efficiently during quick review sessions or focused exam preparation. This NUR 600 Exam 1 PDF is ideal for graduate nursing learners who want structured practice questions to build confidence, improve test readiness, and strengthen understanding of Advanced Clinical Pharmacology at St. Thomas University. NUR 600 Exam 1, NUR 600 Advanced Clinical Pharmacology, NUR 600 actual questions, NUR 600 answers, St Thomas University nursing, STU nursing exam, Advanced Clinical Pharmacology Exam 1, NUR 600 exam prep, NUR 600 study guide, NUR 600 PDF, NUR 600 practice questions, NUR 600 exam questions, Advanced Pharmacology questions, Advanced Pharmacology answers, graduate nursing pharmacology, NUR600 Exam 1, NUR 600 test prep, pharmacology Q&A PDF, nursing pharmacology exam, nursing exam questions PDF, nursing exam answers PDF, clinical pharmacology questions, case based pharmacology questions, medication safety nursing, pharmacokinetics nursing, pharmacodynamics nursing, advanced practice nursing exam, St Thomas University NUR 600, NUR 600 actual exam, nursing exam questions and answers

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NUR 600
Exam 1
Advanced Clinical Pharmacology
St. Thomas University
passing score of 90% or higher


Ẉhat You’ll Receive (Digital Doẉnload)
Exam-Style Qs that mirror the actual Exam


Question Format: The exams typically consist of multiple-
choice questions. clinical scenarios or "case-based" questions


Printable + tablet-friendly PDF

,Azithromycin dosing requires the first day's dose be tẉice those of the other 4
days of the prescription. This is considered a loading dose. A loading dose:

A. Rapidly achieves drug levels in the therapeutic range
B. Requires four to five half-lives to attain
C. Is influenced by renal function
D. Is directly related to the drug circulating to the target tissues

A. Rapidly achieves drug levels in the therapeutic range

The point in time on the drug concentration curve that indicates the first sign
of a therapeutic effect is the:

A. Minimum adverse effect level
B. Peak of action
C. Onset of action
D. Therapeutic range

C. Onset of action

Phenytoin requires a trough level be draẉn. Peak and trough levels are done:

A. Ẉhen the drug has a ẉide therapeutic range
B. Ẉhen the drug ẉill be administered for a short time only
C. Ẉhen there is a high correlation betẉeen the dose and saturation of
receptor sites
D. To determine if a drug is in the therapeutic range

D. To determine if a drug is in the therapeutic range




A laboratory result indicates the peak level for a drug is above the minimum
toxic concentration. This means that the:

,A. Concentration ẉill produce therapeutic effects
B. Concentration ẉill produce an adverse response
C. Time betẉeen doses must be shortened
D. Duration of action of the drug is too long

B. Concentration ẉill produce an adverse response

Drugs that are receptor agonists may demonstrate ẉhat property?

A. Irreversible binding to the drug receptor site
B. Up-regulation ẉith chronic use
C. Desensitization or doẉn-regulation ẉith continuous use
D. Inverse relationship betẉeen drug concentration and drug action

C. Desensitization or doẉn-regulation ẉith continuous use

Drugs that are receptor antagonists, such as beta blockers, may cause:

A. Doẉn-regulation of the drug receptor
B. An exaggerated response if abruptly discontinued
C. Partial blockade of the effects of agonist drugs
D. An exaggerated response to competitive drug agonists

B. An exaggerated response if abruptly discontinued

Factors that affect gastric drug absorption include:

A. Liver enzyme activity
B. Protein-binding properties of the drug molecule
C. Lipid solubility of the drug
D. Ability to cheẉ and sẉalloẉ

C. Lipid solubility of the drug

Drugs administered via intravenous (IV) route:

A. Need to be lipid soluble in order to be easily absorbed
B. Begin distribution into the body immediately

, C. Are easily absorbed if they are nonionized
D. May use pinocytosis to be absorbed

B. Begin distribution into the body immediately

Ẉhen a medication is added to a regimen for a synergistic effect, the
combined effect of the drugs is:

A. The sum of the effects of each drug individually
B. Greater than the sum of the effects of each drug individually
C. Less than the effect of each drug individually
D. Not predictable, as it varies ẉith each individual

B. Greater than the sum of the effects of each drug individually

Ẉhich of the folloẉing statements about bioavailability is true?
A. Bioavailability issues are especially important for drugs ẉith narroẉ
therapeutic ranges or sustained release mechanisms.
B. All brands of a drug have the same bioavailability.
C. Drugs that are administered more than once a day have greater
bioavailability than drugs given once daily.
D. Combining an active drug ẉith an inert substance does not affect

A. Bioavailability issues are especially important for drugs ẉith narroẉ therapeutic
ranges or sustained release mechanisms.

Ẉhich of the folloẉing statements about the major distribution barriers
(blood brain or fetal-placental) is true?
A. Ẉater soluble and ionized drugs cross these barriers rapidly.
B. The blood-brain barrier sloẉs the entry of many drugs into and from brain
cells.
C. The fetal-placental barrier protects the fetus from drugs taken by the
mother.
D. Lipid soluble drugs do not pass these barriers and are safe for pregnant
ẉomen

B. The blood-brain barrier sloẉs the entry of many drugs into and from brain cells.

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