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Robbins Basic Pathology Test Bank — Complete 10th Edition MCQs for Pathophysiology Exam Prep

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Robbins Basic Pathology Test Bank — Complete 10th Edition MCQs for Pathophysiology Exam Prep Description: Master pathology with the definitive Robbins Basic Pathology — 10th Edition test bank: a complete, chapter-by-chapter practice resource engineered to accelerate learning, increase exam confidence, and boost scores on NCLEX, HESI, USMLE, and medical licensing exams. Built for nursing and medical students, this digital package delivers full textbook coverage (ALL chapters) with 20 clinically focused MCQs per chapter, each item including the correct answer and a verified, evidence-based rationale grounded in Robbins’ authoritative pathology framework. Why learners convert to this test bank: it saves study time by organizing high-value practice by chapter, sharpens clinical reasoning with application-level stems, and systematically reinforces disease mechanisms and diagnostic interpretation. Use it for targeted review, timed practice sessions, or instructor-led formative assessment to identify knowledge gaps quickly. Features: • FULL coverage of Robbins Basic Pathology, 10th Edition — ALL chapters. • 20 MCQs per chapter (chapter-indexed for focused study). • Correct answers + verified rationales for every question. • Clinical vignettes emphasizing pathophysiology, diagnostics, and patient-safety decision making. • Ready-to-use for NCLEX, HESI, USMLE, classroom quizzes, and self-study. • Digital format: copy/paste-ready for LMS, printable practice sets, and rapid integration. Authority & trust: Robbins is the global gold standard in pathology education—this test bank aligns directly with its content, giving students a reliable, high-yield way to convert knowledge into exam performance. Keywords: Robbins Basic Pathology test bank pathology MCQs Robbins 10th edition test bank pathophysiology question bank medical exam prep pathology USMLE pathology practice questions NCLEX pathology review HESI pathology test bank Hashtags: #RobbinsPathology #PathologyMCQs #Pathophysiology #MedicalExamPrep #USMLEPrep #NCLEXPrep #HESIReview #TestBank #MedicalEducation #StudySmart

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Uploaded on
November 3, 2025
Number of pages
704
Written in
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 unexplained recurrent thrombosis
undergoes genomic testing that shows a single-nucleotide
polymorphism (SNP) in a regulatory noncoding region near a
coagulation gene. Which mechanism best explains how the SNP
could increase thrombosis risk?
Options
A. The SNP creates a novel protein with procoagulant activity.
B. The SNP disrupts transcription factor binding and increases
gene expression.

,C. The SNP deletes a coding exon leading to a truncated
coagulation protein.
D. The SNP increases mitochondrial DNA replication in
hepatocytes.
Correct answer
B
Rationales
Correct (B): Noncoding variants (including SNPs in regulatory
regions) commonly alter transcription factor binding or
enhancer activity, changing expression of nearby genes and
thereby affecting phenotype. This mechanism explains
increased procoagulant protein levels and thrombosis risk.
Incorrect (A): SNPs in noncoding regions do not create novel
proteins because they are not translated.
Incorrect (C): Deleting a coding exon is a structural coding
mutation (large deletion), not an isolated regulatory SNP.
Incorrect (D): Mitochondrial DNA replication changes are
unrelated to a nuclear regulatory SNP near a coagulation gene.
Teaching point
Noncoding variants can alter gene expression by changing
regulatory element activity.
Citation (simplified APA)
Kumar et al. (2017). Robbins Basic Pathology (10th Ed.). Ch. 1.
Scribd+1

,2
Reference – Ch. 1 — The Genome
Question stem
A patient’s tumor sequencing reveals amplification of a proto-
oncogene caused by a copy number variant (CNV). Which
cellular consequence most directly follows CNV-driven proto-
oncogene amplification?
Options
A. Loss of heterozygosity and reduced protein expression.
B. Increased mRNA and protein expression of the proto-
oncogene.
C. Increased microRNA repression of tumor suppressors.
D. Enhanced lysosomal degradation of the proto-oncogene
protein.
Correct answer
B
Rationales
Correct (B): Gene amplification (a CNV) increases copy number,
typically raising mRNA transcription and protein levels of the
amplified gene, which can drive oncogenic signaling.
Incorrect (A): Loss of heterozygosity denotes deletion of a
functional allele, not amplification.
Incorrect (C): microRNA repression is a post-transcriptional
regulatory mechanism but is not the direct result of DNA
amplification.

, Incorrect (D): Lysosomal degradation is a protein degradation
pathway and is not a direct consequence of increased gene
copy number.
Teaching point
Copy number gains raise gene dosage → increased mRNA and
protein expression.
Citation (simplified APA)
Kumar et al. (2017). Robbins Basic Pathology (10th Ed.). Ch. 1.
Scribd+1


3
Reference – Ch. 1 — The Genome
Question stem
A neonate with multiple congenital anomalies is found to have
abnormal histone modification patterns on chromatin analysis.
Which downstream effect best explains how altered histone
modification produces abnormal tissue development?
Options
A. Immediate cleavage of mRNA transcripts.
B. Changes in chromatin accessibility altering gene transcription
during development.
C. Sudden changes in mitochondrial oxidative phosphorylation.
D. Increased proteasomal degradation of DNA.
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