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Robbins Basic Pathology Test Bank — 10th Edition | 20 MCQs/Chapter • Answers & Verified Rationales • Pathophysiology Exam Prep

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Robbins Basic Pathology Test Bank — 10th Edition | 20 MCQs/Chapter • Answers & Verified Rationales • Pathophysiology Exam Prep Description: Master pathology with the ultimate digital study companion built for nursing and medical students: the complete Robbins Basic Pathology — 10th Edition Test Bank. This professionally curated resource delivers FULL textbook coverage with 20 clinically focused MCQs per chapter, each question paired with the single-best answer and evidence-based, exam-ready rationales. Designed to accelerate learning, reduce study time, and build unshakeable confidence for high-stakes exams (NCLEX, HESI, USMLE, shelf exams, and school assessments). What you get: a comprehensive, chapter-mapped question bank that reinforces disease mechanisms, diagnostic reasoning, and patient-safety decision making—mirroring Robbins’ gold-standard pathology content and terminology. Questions emphasize applied clinical reasoning and exam-style format to boost retention and performance on pathophysiology topics across systems. Benefits: Save time with pre-made, chapter-aligned practice questions Improve exam scores via targeted retrieval practice and rationale review Deepen understanding of mechanisms, diagnostics, and clinical correlation Use for focused review sessions, mock exams, or curriculum integration Features: Complete coverage of all Robbins Basic Pathology 10th Ed. chapters 20 MCQs per chapter (single-best-answer format) Correct answers + verified, concise rationales for every item Clinically oriented vignettes emphasizing safety and decision-making Downloadable digital format for instant access and offline study Backed by Robbins’ global reputation, this test bank is the efficient, high-yield path to pathology mastery and measurable exam success. Keywords: Robbins Basic Pathology test bank pathology MCQs Robbins 10th edition questions pathophysiology test bank medical exam prep pathology NCLEX pathology practice USMLE pathology question bank HESI pathology questions Hashtags: #RobbinsBasicPathology #PathologyMCQs #Pathophysiology #TestBank #NCLEXPrep #HESIPrep #USMLEPrep #MedicalEducation #NursingStudyResources #ExamPractice

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2025/2026
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Robbins Basic Pathology
10th Edition


Author(s)Vinay Kumar; Abul K. Abbas;
Jon C. Aster



TEST BANK

1)
Reference — Ch. 1 — The Genome
Question Stem
A 28-year-old woman with progressive sensorineural hearing
loss has children with variable severity of the same disorder.
Which genomic feature best explains the variable expression
seen among her offspring?
Options
A. Autosomal dominant transmission with incomplete
penetrance
B. Heteroplasmy of mitochondrial DNA mutations

,C. X-linked recessive transmission with lyonization in daughters
D. Anticipation caused by trinucleotide repeat expansion
Correct Answer: B
Rationales
• B (Correct): Mitochondrial DNA mutations are maternally
inherited and often present with heteroplasmy (mixture of
mutant and normal mtDNA) that produces variable
severity among offspring.
• A: Incomplete penetrance can cause variable expression
but would not explain consistent maternal transmission to
all children.
• C: X-linked recessive disorders have different transmission
patterns (typically males more affected); lyonization
explains variability in females but not maternal-only
inheritance to both sexes.
• D: Anticipation explains progressive earlier onset across
generations for repeat expansion disorders, not the
variable severity among siblings from the same mother.
Teaching Point
Mitochondrial heteroplasmy causes variable disease
expression in maternally inherited disorders.
Citation
Kumar et al. (2021). Robbins Basic Pathology (10th Ed.).
Ch. 1.

,2)
Reference — Ch. 1 — Cellular Housekeeping
Question Stem
A patient receives a proteasome inhibitor for multiple myeloma.
Which cellular consequence most directly results from
proteasome inhibition and contributes to myeloma cell death?
Options
A. Increased lysosomal degradation of organelles
B. Accumulation of ubiquitinated proteins leading to ER stress
and apoptosis
C. Enhanced autophagic flux that clears misfolded proteins
D. Increased mitochondrial biogenesis to meet ATP demand
Correct Answer: B
Rationales
• B (Correct): Proteasome inhibition causes buildup of
ubiquitinated/misfolded proteins in the cytoplasm and ER,
inducing ER stress and apoptotic pathways—therapeutic in
myeloma.
• A: Lysosomal degradation is separate from proteasomal
degradation; proteasome inhibition does not increase
lysosomal breakdown.
• C: In some cases autophagy may be induced as
compensation but proteasome inhibition primarily causes
accumulation rather than enhanced clearance.
• D: Proteasome inhibition does not directly stimulate
mitochondrial biogenesis to resolve protein accumulation.

, Teaching Point
Proteasome inhibition → ubiquitinated protein
accumulation → ER stress → apoptosis.
Citation
Kumar et al. (2021). Robbins Basic Pathology (10th Ed.).
Ch. 1.


3)
Reference — Ch. 1 — Cellular Metabolism and Mitochondrial
Function
Question Stem
A 56-year-old man develops exercise intolerance and lactic
acidosis after a suspected defect in mitochondrial oxidative
phosphorylation. Which of the following best explains why
tissues with high energy demand are most affected?
Options
A. High-demand tissues rely primarily on anaerobic glycolysis at
baseline
B. Mitochondrial defects impair ATP generation via oxidative
phosphorylation, especially in high-ATP–requiring tissues
C. Mitochondrial DNA mutations are selectively expressed in
skeletal muscle only
D. Mitochondrial dysfunction increases peroxisomal β-
oxidation, depleting energy substrates
Correct Answer: B
Rationales
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