WBR0116
| Author | [[PageAuthor::Mahmoud Sakr (Reviewed by Will J Gibson, Rim Halaby, M.D. [1], and Yazan Daaboul, M.D.)]] | ||||||||||
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| Exam Type | ExamType::USMLE Step 1 | ||||||||||
| Main Category | MainCategory::Genetics | ||||||||||
| Sub Category | SubCategory::Gastrointestinal | ||||||||||
| Prompt | [[Prompt::A 33-year-old Caucasian female presents with complaints of diarrhea and foul-smelling bulky stools for the past 3 weeks. She previously tried several over-the-counter medications with no relief. Yesterday, she noticed an eruption of intensely pruritic papules and vesicles on her elbows, dorsal forearms, and back. She recalls that her older brother has suffered from a similar illness for approximately 5 years. Her blood pressure is 120/80 mmHg, heart rate is 70/min, and temperature is 36.8 °C (98.24 °F). Routine laboratory work-up is ordered and is unremarkable. Serologic testing revealed elevated levels of tissue transglutaminase IgA antibodies. Which of the following gene mutations most likely predisposed this patient to develop his condition?]] | ||||||||||
| Answer A | AnswerA::HLA DQ2 gene | ||||||||||
| Answer A Explanation | [[AnswerAExp::This patient suffers from celiac disease or gluten-sensitive enteropathy, which is genetically predisposed by HLA DQ2 or HLA DQ8 gene subtypes.]] | ||||||||||
| Answer B | AnswerB::IBD1 gene | ||||||||||
| Answer B Explanation | AnswerBExp::IBD1 encodes an intracellular pattern recognition receptor (NOD2). IBD1 mutations are associated with inflammatory bowel diseases. | ||||||||||
| Answer C | AnswerC::HLA-DR2 | ||||||||||
| Answer C Explanation | [[AnswerCExp::The HLA-DR2 variant is associated with inflammatory bowel disease.]] | ||||||||||
| Answer D | AnswerD::APC gene | ||||||||||
| Answer D Explanation | [[AnswerDExp::APC gene mutations predispose to familial adenomatous polyposis. APC encodes a gene that functions to degrade the transcription factor beta-catenin.]] | ||||||||||
| Answer E | AnswerE::MSH2 gene | ||||||||||
| Answer E Explanation | [[AnswerEExp::MSH2 gene mutation is associated with Hereditary nonpolyposis colorectal cancer. MSH2 encodes a DNA mismatch repair enzyme.]] | ||||||||||
| Right Answer | RightAnswer::A | ||||||||||
| Explanation | [[Explanation::Celiac disease is an autoimmune disease of the small intestine that occurs among genetically predisposed individuals of all ages. The onset of symptoms is typically during late childhood or early adulthood. Symptoms include abdominal pain and discomfort, chronic diarrhea, failure to thrive in children, anemia and fatigue. Although abdominal symptoms may be absent, symptoms in other organ systems could also be present.
Antibodies against tissue transglutaminase are present in nearly all individuals with celiac disease. Serology for anti-tTG antibodies has superseded older serological tests (anti-endomysium, anti-gliadin, and anti-reticulin) and has a strong sensitivity (99%) and specificity (>90%) for identifying celiac disease. The greatest risk factor for celiac disease is another family member with celiac disease. The second most influential risk factor is the presence of the HLA-DQ2 subtype. Celiac disease is genetically predisposed by HLA-DQ2 or HLA-DQ8 HLA subtypes. While these HLA subtypes are present in ~30% of individuals of European descent, only 1% of the population develops celiac disease (Hunt et al). HLA associations are commonly tested on the USMLE. One useful mnemonic for the HLA associations is DR = MD..AAH
Educational Objective: Celiac disease is genetically predisposed by HLA-DQ2 or HLA-DQ8 HLA subtypes. Hunt KA, Zhernakova A, Turner G, et al. Newly identified genetic risk variants for celiac disease related to the immune response. Nat Genet. 2008;40(4):395-402.]] | ||||||||||
| Approved | Approved::Yes | ||||||||||
| Keyword | WBRKeyword::Celiac disease; HLA-DQ2; HLA-DQ8; HLA; diarrhea; chronic diarrhea; HLA; | ||||||||||
| Linked Question | Linked:: | ||||||||||
| Order in Linked Questions | LinkedOrder:: |