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Mastering Robbins Pathology (10th Ed.) — Comprehensive Chapterwise Q-Bank for Board & Certification Prep

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Robbins & Cotran 10th Ed. — Complete Chapter-by-Chapter Test Bank: Verified Answers & Evidence-Based Rationales Mastering Robbins Pathology (10th Ed.) — Comprehensive Chapterwise Q-Bank for Board & Certification Prep High-converting Stuvia product description (ready to paste) Product title: Robbins & Cotran 10th Ed. — Complete Chapter-by-Chapter Test Bank: Verified Answers & Evidence-Based Rationales Short subtitle: 2,500+ exam-style questions mapped to every Robbins chapter — clinical vignettes, verified answers, and concise pathophysiology rationales. Long description (marketing + features): Prepare faster and smarter with the most comprehensive Robbins & Cotran (10th edition) chapter-by-chapter test bank available on Stuvia. Designed by expert item-writers in pathology and medical education, this Q-bank delivers realistic, exam-style multiple-choice questions and clinical vignettes mapped directly to each Robbins chapter. Every question includes a verified correct answer and a succinct, evidence-based rationale tied to Robbins’ core mechanisms — perfect for medical students, residents, and clinicians preparing for board and licensing exams. What you get: Complete chapter mapping: Questions aligned to every Robbins chapter for focused, efficient study. Verified correct answers + rationales: Clear, mechanism-based explanations that cite core Robbins concepts to reinforce understanding. Exam-style vignettes: Clinical stems that mimic USMLE/PLAB/other board formats to build application skills. Multiple item formats: Single-best-answer MCQs, clinical reasoning items, and item writers’ tips for distractor design. Study aids included: Chapter quizzes, cumulative practice tests, answer key CSV, and printable PDF. Certification-aligned focus: Questions emphasize high-yield concepts commonly tested on board and licensure exams. Flexible use: Self-study, group review, classroom use, and instructor test construction. Why learners love it: Questions are written by pathology educators with Robbins expertise — concise rationales make every item a mini-lesson so you learn while you test. Designed to maximize exam readiness and retention, not just rote memorization. Important note: This resource is an evidence-based study aid intended to strengthen knowledge and exam technique. While it is designed to significantly improve preparedness, no study material can absolutely guarantee certification outcomes. #RobbinsPathology #PathologyQBank #Robbins10thEd #MedicalExamPrep #USMLEPrep #BoardExamQuestions #PathologyMCQs #ClinicalVignettes #MedicalStudents #ExamReady 8 SEO keywords (high relevance) Robbins & Cotran 10th edition test bank pathology MCQs with rationale chapter by chapter Robbins questions pathology question bank for boards Robbins pathology Q-bank PDF USMLE pathology practice questions evidence-based pathology exam prep comprehensive pathology Qbank

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Subido en
15 de septiembre de 2025
Número de páginas
626
Escrito en
2025/2026
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Examen
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Robbins & Cotran 10th Ed. Pathology Test Bank | Chapter-
by-Chapter Questions & Verified Solutions




Robbins & Cotran Pathologic Basis of Disease
10th Edition
• Author(s)Vinay Kumar; Abul K. Abbas; Jon C. Aster
Chapter Reference – Chapter 1: The Cell as a Unit of Health
and Disease
The Genome
Cellular Housekeeping
Cellular Metabolism and Mitochondrial Function
Cellular Activation
Growth Factors and Receptors
Extracellular Matrix
Maintaining Cell Populations
Stem: A 45-year-old man with early-onset colorectal cancer is
found to have numerous insertion–deletion mutations at short
tandem repeat loci (microsatellites). Which DNA repair defect
most directly explains these findings?
A. Defective nucleotide excision repair (NER)
B. Defective base excision repair (BER)

,C. Defective DNA mismatch repair (MMR)
D. Defective homologous recombination (double-strand break
repair)
Correct Answer – C
Rationales
• Correct (C): DNA mismatch repair corrects replication
slippage errors at microsatellites; defects produce
microsatellite instability and predispose to colorectal
cancers (Lynch syndrome).
• Incorrect (A): NER repairs bulky helix-distorting lesions
(e.g., UV dimers), not replication slippage at
microsatellites.
• Incorrect (B): BER repairs small base modifications
(oxidation, alkylation), not microsatellite replication errors.
• Incorrect (D): Homologous recombination repairs double-
strand breaks; its defect leads to chromosomal instability
rather than microsatellite instability.
Teaching Point: Mismatch repair deficiency causes
microsatellite instability and increases colorectal cancer risk.


2
Chapter Reference – Chapter 1: The Cell as a Unit of Health
and Disease
The Genome

,Cellular Housekeeping
Cellular Metabolism and Mitochondrial Function
Cellular Activation
Growth Factors and Receptors
Extracellular Matrix
Maintaining Cell Populations
Stem: A patient exposed to cyanide develops profound lactic
acidosis and tissue hypoxia despite normal arterial oxygen
content. Which mitochondrial target is inhibited by cyanide to
produce this metabolic picture?
A. Complex I (NADH dehydrogenase)
B. Complex II (succinate dehydrogenase)
C. Complex III (cytochrome bc1)
D. Complex IV (cytochrome c oxidase)
Correct Answer – D
Rationales
• Correct (D): Cyanide binds to cytochrome c oxidase
(Complex IV), blocking electron transfer to oxygen, halting
oxidative phosphorylation and increasing anaerobic
glycolysis and lactate.
• Incorrect (A): Complex I inhibition causes similar effects
but cyanide specifically targets Complex IV.
• Incorrect (B): Complex II feeds electrons from succinate
but is not cyanide’s primary target.

, • Incorrect (C): Complex III inhibition impairs respiration, but
cyanide acts at Complex IV.
Teaching Point: Inhibition of Complex IV blocks final electron
transfer, causing anaerobic metabolism and lactic acidosis.


3
Chapter Reference – Chapter 1: The Cell as a Unit of Health
and Disease
The Genome
Cellular Housekeeping
Cellular Metabolism and Mitochondrial Function
Cellular Activation
Growth Factors and Receptors
Extracellular Matrix
Maintaining Cell Populations
Stem: Neurons in a patient with a familial neurodegenerative
syndrome show accumulation of ubiquitinated protein
aggregates. Which cellular system normally disposes of
ubiquitinated misfolded proteins?
A. Autophagy–lysosomal pathway
B. Ubiquitin–proteasome system (UPS)
C. Endoplasmic reticulum-associated degradation (ERAD)
without ubiquitination
D. Exosome secretion
Correct Answer – B
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