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NCLEX NGN SULFA NIGHTMARE: 320 Q&A on Crystalluria, G6PD Crisis & Deadly Adverse Effects (SJS, Hemolysis, Renal Tox) Next Gen Clinical Judgment + Pharm Mastery - IDSA/NIH Guidelines & Case-Based MCQs/SATA

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Infectious Disease / Drug Allergy
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Infectious Disease / Drug Allergy

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Uploaded on
June 18, 2025
Number of pages
106
Written in
2024/2025
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Exam (elaborations)
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Section 1: Sulfonamide Pharmacology & Crystalluria


I. Multiple Choice Questions (40 Total)


Questions 1-20


1. What biochemical property of sulfonamide metabolites primarily

drives crystalluria?

A) High solubility in lipids

B) Low solubility in acidic urine

C) Strong protein-binding affinity

D) Rapid glomerular filtration

Answer: B

Rationale: Sulfonamides are acetylated in the liver into metabolites

like N-acetyl-sulfamethoxazole, which exhibit poor solubility in acidic

environments (pH < 5.5). These metabolites precipitate as needle-shaped

crystals in renal tubules, causing mechanical obstruction and acute

kidney injury. This pH-dependent insolubility is distinct from other

nephrotoxins and underscores the need for urine alkalinization per

Katzung’s Pharmacology (15th ed., Ch. 46).

2. Which patient is at HIGHEST risk for sulfonamide crystalluria?

A) A 25-year-old athlete on TMP-SMX with urine pH 7.2

B) A 70-year-old with heart failure (on fluid restriction) and urine pH 5.0

C) A 40-year-old taking sodium bicarbonate with urine output 2L/day

, 3


D) A 30-year-old with asthma using albuterol

Answer: B

Rationale: Advanced age, dehydration from fluid restriction, and acidic

urine (pH 5.0) synergistically increase crystalluria risk. Reduced urine

volume concentrates sulfonamide metabolites, while low pH promotes

precipitation. IDSA UTI Guidelines (2021) flag elderly patients with

comorbidities as "high-risk," requiring aggressive hydration and pH

monitoring. Neither asthma (D) nor alkalinization (C) confers significant

risk.

3. Urine alkalinization with sodium bicarbonate prevents crystalluria

by:

A) Increasing the ionization of sulfonamide metabolites

B) Enhancing renal blood flow

C) Inhibiting hepatic acetylation

D) Chelating calcium in urine

Answer: A

Rationale: Alkalinization (target pH 7.0–7.5) ionizes sulfonamide

metabolites, converting them into water-soluble forms that resist

precipitation. This does not alter hepatic metabolism or renal perfusion

but directly enhances solubility. Rang & Dale’s Pharmacology (2023)

notes that sodium bicarbonate is preferred over citrate in renal

impairment due to no potassium load.

, 4


4. Which sulfonamide is MOST associated with crystalluria?

A) Sulfasalazine (for IBD)

B) Sulfadiazine (for toxoplasmosis)

C) Sulfamethoxazole (in TMP-SMX)

D) Acetazolamide (for glaucoma)

Answer: B

Rationale: Sulfadiazine has the lowest solubility of common

sulfonamides, especially in acidic urine, and is used in high doses for

CNS infections. Its acetylated metabolite rapidly forms stable crystals,

necessitating strict hydration (>3L/day) and alkalinization.

Sulfamethoxazole (C) has higher solubility, while non-antibiotic agents

(A, D) rarely cause crystalluria (Katzung’s, 15th ed.).

5. A patient develops sulfonamide crystalluria. Urine microscopy would

MOST likely show:

A) Hexagonal crystals

B) Rhomboid crystals

C) Needle-shaped crystals

D) Amorphous crystals

Answer: C

Rationale: Sulfonamide metabolites (e.g., acetyl-sulfadiazine) form

needle-shaped or sheaf-like crystals under microscopy, distinct from uric

acid (rhomboid) or cystine (hexagonal) crystals. This morphology is
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