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NR 567 – Advanced Pharmacology | Midterm Exam Study Guide (2026/2027) – Verified Questions and Correct Answers | Grade A

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This document contains the complete NR 567 Midterm Exam Study Guide for the 2026/2027 academic year, featuring verified questions and correct answers. It covers core topics in advanced pharmacology including pharmacokinetics, pharmacodynamics, drug classifications, adverse reactions, contraindications, and clinical application of medications across various systems. Perfect for nurse practitioner students seeking a comprehensive and reliable review to prepare for the NR 567 midterm exam. 1. What laboratory parameters should be monitored when administering thrombolytics?: CBC, PT/INR, and PTT. 2. What is the recommended dosing for alteplase in acute myocardial infarction (MI)?: 100 mg total: 15 mg IV bolus, 50 mg over 30 minutes, and 35 mg over 60 minutes. 3. What is the bioavailability of alteplase when administered IV?: 100% due to IV administration. 4. How is alteplase metabolized?: Rapid hepatic clearance, mainly by the liver through internalization and catabolism by hepatic cells. 5. What is the initial elimination half-life of alteplase?: About 5 minutes (rapid plasma clearance).

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Uploaded on
September 26, 2025
Number of pages
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Written in
2025/2026
Type
Exam (elaborations)
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Questions & answers

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1
NR 567 Midterm




NR 567 Midterm Exam Study Guide for Advanced
Pharmacology Questions with Correct Verified
Answers (Latest 2026/2027)




1.What laboratory parameters should be monitored when administering

thrombolytics?: CBC, PT/INR, and PTT.

2.What is the recommended dosing for alteplase in acute myocardial infarction

(MI)?: 100 mg total: 15 mg IV bolus, 50 mg over 30 minutes, and 35 mg over

60 minutes.

3.What is the bioavailability of alteplase when administered IV?: 100% due to

IV administration.

4.How is alteplase metabolized?: Rapid hepatic clearance, mainly by the liver

through internalization and catabolism by hepatic cells.

5.What is the initial elimination half-life of alteplase?: About 5 minutes (rapid

plasma clearance).




NR 567 Midterm

, .


6.What is the terminal elimination half-life of alteplase?: About 35-50 minutes

(slower elimination).

7.What is the mechanism of action of statins like lovastatin?: Statins inhibit

HMG-CoA reductase in the liver, reducing cholesterol synthesis and lowering

LDL cholesterol levels.

8.What are the medications used in acute pulmonary embolism?: Heparin and

alteplase (Activase).

16 What is the recommended dosage of alteplase for pulmonary embolism?:

100 mg infused IV over 2 hours.

17. What are the side effects and adverse effects of thrombolytics?:

Bleeding, including major bleeding risks and intracranial hemorrhage.

18. What precautions should be taken when administering thrombolytics?:

Monitor for contraindications such as prior intracranial hemorrhage and

active internal bleeding.

19. What is the route of administration for alteplase?: IV only.






, .


20. What is the significance of monitoring coagulation parameters in patients

receiving thrombolytics?: To assess bleeding risk and ensure safe

administration.

21. What is the pharmacokinetic property of alteplase regarding its

distribution?: It is mostly distributed in plasma.

22. What are the key concepts to remember regarding drug classes in this

course?: Know the drug class and individual generic drug names, mechanisms

of action, pharmacokinetics, side effects, and contraindications.

23. What is the time frame for monitoring after administering

thrombolytics?: -

Continuous monitoring for signs of bleeding and changes in coagulation

parameters.

24. What is the importance of understanding pharmacodynamics in drug

administration?: It helps predict how the drug affects the body and informs

safe and effective dosing.






, .


25. What is the primary use of statins after myocardial infarction (MI)?: To

reduce the risk of death, recurrent myocardial infarction, and

thromboembolic events such as stroke or systemic embolization.

26. What are the potential side effects of statins?: Hepatotoxicity, myopathy,

and rhabdomyolysis.

27. What does hepatotoxicity indicate in patients taking statins?: Increased

liver enzymes indicating potential liver damage.

28. What should be monitored to assess muscle breakdown in patients on

statins?: CK lab values.

29. What precautions should be taken before starting statin treatment?:

Perform liver function tests prior to initiating treatment and when clinically

indicated.

30. Why should statins be used cautiously in elderly clients?: Due to an

increased risk of muscle-related side effects.

31. What specific consideration should be made for clients of Asian descent

regarding statin use?: Certain statins, particularly rosuvastatin, may cause

toxicity due to altered metabolism. 32 What drug interactions should be

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