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NURS 5433 Module 3 Exam QUESTIONS AND ANSWERS ALREADY GRADED A+. 100% Verified Solutions | Updated Per Latest Guidelines | Graded A

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This exam preparation document for NURS 5433 Module 3 at the University of Texas at Arlington is meticulously crafted to provide nursing students with a rigorous review of advanced nursing concepts. The 250 verified questions are organized by content area, each with detailed rationales and distractor analyses that promote critical thinking and clinical reasoning. The material aligns with the 2026/2027 academic year standards, incorporating the latest evidence-based practices and regulatory updates. By systematically addressing pathophysiology, pharmacology, assessment, and ethical issues, this guide ensures comprehensive coverage of module objectives. Students who engage with this resource will develop a deeper understanding of complex nursing scenarios, ultimately achieving a graded A+ performance on the exam. The document's structured approach facilitates efficient study and retention, making it an indispensable tool for exam success

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Institution
Nurs 5433
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NURS 5433 Module 3 Exam Prep Document | 2026/2027
Edition | 250 Verified Questions
NURS 5433 Module 3 Exam 2026-2027 QUESTIONS AND ANSWERS ALREADY GRADED
A+. 100% Verified Solutions | Updated Per Latest Guidelines | Graded A+
This comprehensive exam preparation guide for NURS 5433 Module 3 at the University of Texas at
Arlington contains 250 verified questions covering all key content areas. Designed to ensure a 100%
pass rate, this resource reflects the latest 2026/2027 curriculum updates and evidence-based practice
guidelines. Each question includes detailed rationales and distractors to reinforce learning and critical
thinking. Ideal for students seeking a complete A+ guide to master the module exam.


Key Features:
Advanced Pathophysiology and Disease Mechanisms
Pharmacological Interventions and Drug Calculations
Clinical Assessment and Diagnostic Reasoning
Patient Safety and Quality Improvement
Ethical and Legal Considerations in Nursing
Evidence-Based Practice and Research Integration
Updates for 2026:
- Updated to reflect 2026/2027 curriculum changes
- Incorporated latest evidence-based practice guidelines
- Revised rationales for clarity and accuracy
- Added new questions on emerging healthcare topics
- Enhanced distractor explanations for deeper understanding
Abstract:
This exam preparation document for NURS 5433 Module 3 at the University of Texas at Arlington is meticulously
crafted to provide nursing students with a rigorous review of advanced nursing concepts. The 250 verified
questions are organized by content area, each with detailed rationales and distractor analyses that promote
critical thinking and clinical reasoning. The material aligns with the 2026/2027 academic year standards,
incorporating the latest evidence-based practices and regulatory updates. By systematically addressing
pathophysiology, pharmacology, assessment, and ethical issues, this guide ensures comprehensive coverage of
module objectives. Students who engage with this resource will develop a deeper understanding of complex nursing
scenarios, ultimately achieving a graded A+ performance on the exam. The document's structured approach
facilitates efficient study and retention, making it an indispensable tool for exam success.
Keywords:
NURS 5433, Module 3 Exam, University of Texas Arlington, Nursing Exam Prep, 250 Questions, A+ Guide,
Evidence-Based Practice, Pathophysiology
Answer Format:
Each question is followed by the correct answer, a detailed rationale explaining the underlying concept, and an
analysis of incorrect distractors to clarify common misconceptions. This format reinforces learning and helps
students understand why each option is correct or incorrect.
Compliance Checklist:
Aligned with 2026/2027 NURS 5433 curriculum
Verified by subject matter experts
Includes evidence-based rationales




Page 1

, Covers all module learning objectives
Updated per latest nursing guidelines
Designed for 100% pass rate guarantee

Content Area Overview:

Content Area Questions Key Topics Weight

Advanced Pathophysiology 1-50 Cellular adaptation, inflammation, 20%
hemodynamic disorders, neoplasia, genetic
disorders
Pharmacology 51-100 Pharmacokinetics, pharmacodynamics, 20%
adverse drug reactions, drug interactions,
dosage calculations
Clinical Assessment 101-150 Health history, physical examination, 20%
diagnostic tests, clinical reasoning,
differential diagnosis
Patient Safety & Quality 151-200 Error prevention, infection control, fall 20%
prevention, quality improvement,
patient-centered care
Ethical & Legal Issues 201-250 Informed consent, confidentiality, advance 20%
directives, ethical dilemmas, legal standards




Page 2

,Q1. A patient with type 2 diabetes and chronic kidney disease (eGFR 35 mL/min/1.73m²) is currently on
metformin 1000 mg BID and glipizide 10 mg daily. HbA1c is 8.2%. According to current guidelines, which of
the following adjustments is most appropriate?
A. Continue metformin at current dose and add dapagliflozin.
B. Discontinue metformin and initiate insulin glargine.
C. Reduce metformin to 500 mg BID and add liraglutide.
D. Discontinue metformin and start canagliflozin.
Correct Answer: B. Discontinue metformin and initiate insulin glargine.
Rationale: Metformin is contraindicated when eGFR < 30 mL/min/1.73m² and should be reduced or discontinued
at eGFR 30-45 due to lactic acidosis risk. Dapagliflozin and canagliflozin are SGLT2 inhibitors that lose efficacy
as eGFR declines and are not recommended if eGFR < 45. Liraglutide is not first-line in advanced CKD. Insulin
glargine is appropriate for glycemic control without renal dose adjustment.
Why Wrong:
A - Metformin should be reduced or discontinued at eGFR 30-45, and dapagliflozin is not recommended
when eGFR < 45.
C - Liraglutide is not preferred in advanced CKD and metformin still poses risk at reduced dose.
D - Canagliflozin is not recommended when eGFR < 45 and metformin must be stopped.
Reference: American Diabetes Association. (2025). Standards of Medical Care in Diabetes-2025. Diabetes Care,
48(Suppl 1), S1-S264.

Q2. A patient is admitted with septic shock. Blood cultures grow methicillin-resistant Staphylococcus aureus
(MRSA). The patient has a reported severe allergy to penicillin (anaphylaxis). Which of the following
antibiotic regimens is most appropriate?
A. Vancomycin plus cefepime
B. Daptomycin plus aztreonam
C. Linezolid plus piperacillin-tazobactam
D. Clindamycin plus gentamicin
Correct Answer: B. Daptomycin plus aztreonam
Rationale: For MRSA in septic shock, vancomycin or daptomycin are first-line. However, cefepime has a
beta-lactam ring and may cause cross-reactivity in severe penicillin allergy, so it is avoided. Aztreonam is a
monobactam with minimal cross-reactivity and is safe in penicillin-allergic patients. Daptomycin is effective
against MRSA. Linezolid plus piperacillin-tazobactam includes a beta-lactam (piperacillin) which is
contraindicated in severe penicillin allergy. Clindamycin is not reliable for MRSA bacteremia, and gentamicin is
not adequate monotherapy.
Why Wrong:
A - Cefepime is a cephalosporin with potential cross-reactivity in severe penicillin allergy; vancomycin alone
is insufficient for gram-negative coverage.
C - Piperacillin-tazobactam is contraindicated in severe penicillin allergy.
D - Clindamycin is not recommended for MRSA septic shock; gentamicin is not primary therapy.
Reference: Kaline, K. et al. (2025). Surviving Sepsis Campaign Guidelines. Critical Care Medicine, 53(1), e1-e50.

Q3. A patient with atrial fibrillation (CHADS2-VASc = 4) is on warfarin. INR is 2.0. A new prescription for
amiodarone is initiated for rhythm control. What is the most appropriate management of warfarin therapy?
A. Continue warfarin at same dose and monitor INR weekly.
B. Reduce warfarin dose by 25-50% and monitor INR closely.
C. Hold warfarin for 3 days and then resume at half the dose.
D. Switch to apixaban 5 mg BID.
Correct Answer: B. Reduce warfarin dose by 25-50% and monitor INR closely.
Rationale: Amiodarone is a potent inhibitor of CYP2C9 and warfarin metabolism, leading to increased INR and




Page 3

, bleeding risk. The warfarin dose should be reduced by 25-50% upon amiodarone initiation with close INR
monitoring (every few days until stable). Continuing the same dose risks supratherapeutic INR. Holding warfarin
could cause loss of anticoagulation. Switching to apixaban is an option but not the most appropriate immediate
management; warfarin can be continued with dose adjustment.
Why Wrong:
A - Amiodarone increases warfarin effect; same dose would likely raise INR excessively.
C - Holding warfarin for 3 days may lead to subtherapeutic INR and increased stroke risk.
D - Switching to apixaban is reasonable but not the most appropriate immediate management; dose reduction and
monitoring is standard.

Reference: January, C.T. et al. (2023). AHA/ACC/HRS Guideline for the Management of Atrial Fibrillation. Circulation,
148(1), e1-e100.

Q4. A patient with hypertension (BP 148/92 mmHg) and no other comorbidities is started on lisinopril. After
2 weeks, BP is 142/88 mmHg. The patient develops a dry cough. Which of the following is the most
appropriate next step?
A. Add a thiazide diuretic to lisinopril.
B. Switch lisinopril to losartan.
C. Discontinue lisinopril and start amlodipine.
D. Continue lisinopril and prescribe an antitussive.
Correct Answer: B. Switch lisinopril to losartan.
Rationale: ACE inhibitor-induced cough is a class effect due to bradykinin accumulation. Switching to an
angiotensin receptor blocker (ARB) like losartan provides similar antihypertensive efficacy without the cough, as
ARBs do not affect bradykinin. Adding a thiazide or switching to amlodipine are options but not first-line when the
cough is intolerable. Continuing lisinopril with an antitussive is inappropriate because the cough is drug-related
and will persist.
Why Wrong:
A - Adding a thiazide does not address the cough and may cause additional side effects.
C - Switching to amlodipine is reasonable but not preferred; ARB is a direct substitute.
D - The cough is drug-induced; continuing lisinopril with antitussive is not standard practice.
Reference: Whelton, P.K. et al. (2022). ACC/AHA Guideline for the Prevention, Detection, Evaluation, and
Management of High Blood Pressure. Hypertension, 79(5), e1-e100.

Q5. A patient with major depressive disorder is started on sertraline. After 4 weeks, there is minimal
improvement. The patient reports no significant side effects. Which of the following is the most appropriate
next step?
A. Increase sertraline dose to maximum recommended.
B. Switch to a different SSRI (e.g., escitalopram).
C. Add bupropion as augmentation therapy.
D. Discontinue sertraline and start a monoamine oxidase inhibitor (MAOI).
Correct Answer: A. Increase sertraline dose to maximum recommended.
Rationale: After 4 weeks of SSRI therapy at a standard dose, if response is inadequate and tolerability is good, the
first step is to titrate to the maximum recommended dose over several weeks. Many patients respond at higher
doses. Switching to another SSRI is an option after an adequate trial at maximum dose. Augmentation is considered
after an adequate trial of monotherapy. MAOIs are reserved for treatment-resistant depression due to dietary
restrictions and safety concerns.
Why Wrong:
B - Switching to another SSRI is premature before optimizing dose of current SSRI.
C - Augmentation is considered after failure of adequate monotherapy, not at 4 weeks.
D - MAOIs are not first-line and are reserved for treatment-resistant cases.




Page 4

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