Describe the approach.
Endoscopy, cross-sectional imaging, and laboratory studies are required for the initial evaluation of suspected CD, evaluation of an acute flare, and monitoring response to therapy.
Conduct a thorough history and physical examination (including digital rectal examination).
Document any extraintestinal manifestations of CD.
Evaluate for the presence of perianal fistulas.
Perform endoscopy and obtain intestinal biopsies.
Obtain cross-sectional imaging to:
Establish location(s) and severity of disease
Identify complications (e.g., abscesses, fistulas, strictures)
Obtain laboratory studies (blood and stool) to:
Rule out differential diagnoses of Crohn disease (e.g., infectious gastroenteritis)
Assess and monitor disease activity
Small bowel evaluation is an essential part of the initial diagnostic workup of CD. Almost one-third of patients with CD have only small bowel disease and this may not be visible on ileocolonoscopy.
Describe endoscopy.
Ileocolonoscopy
Indication: all patients with suspected CD
Assesses the distribution and severity of the disease
Aids differentiation of CD from other diseases (e.g., ulcerative colitis)
Monitors disease activity (e.g., active disease, remission)
Can be used therapeutically (e.g., stricture dilatation)
Supportive findings
Skip lesions: segmental and/or discontinuous pattern of involvement (interspersed with normal tissue)
Linear and/or serpiginous ulcerations
Small aphthous ulcerations
Cobblestone sign: inflamed edematous sections interspersed with deep ulcerations that resemble cobblestones
Erythema, fissures, strictures, and fistulas
Discontinuous areas of inflammation, cobblestone appearance of the affected mucosa, and mucosal ulcerations are hallmark endoscopic findings of CD.
Characteristic endoscopic features and evidence of chronic intestinal inflammation on histology are the most important factors to establish a diagnosis of CD.
Describe imaging.
Cross-sectional imaging is preferred as it permits evaluation of the entire gastrointestinal tract (including the small bowel), can identify complications (e.g., bowel obstruction, abscess, fistula), and can assess for differential diagnoses of CD. [16]
Suspected CD (part of initial evaluation)
Localization of inflammation and assessment of severity
Evaluation of suspected acute flare or complications (e.g., abscess)
Serial imaging to assess response to therapy
Modalities and supportive findings
Cross-sectional enterography (MRE, CTE): preferred imaging modality for CD [11][16][20]
Edematous thickening of the intestinal wall
Mucosal enhancement, mesenteric fat stranding
Creeping fat: excessive mesenteric fat around the affected segments of bowel [22]
Can also identify:
Complications (e.g., strictures, fistulas, abscesses)
Extraluminal disease (e.g., cholelithiasis, urolithiasis)
Response to therapy (e.g., healing of ulcers)
Small bowel follow-through : can identify luminal complications such as internal fistulas and narrowed segment(s) of bowel (string sign) [16]
Additional modalities
Ultrasound abdomen
Consider for initial evaluation of suspected CD and for disease monitoring.
Supportive finding (of active disease): bowel wall thickening (> 4 mm)
Plain x-ray abdomen: Consider for expedited assessment of complications
Describe Lab studies.
To rule out differential diagnoses of CD
Stool analysis: to identify ova, cysts, or C. difficile infection in symptomatic patients
Serology: not routinely recommended due to low sensitivity [23]
↑ Anti-Saccharomyces cerevisiae antibodies (ASCA): more commonly elevated in CD than in UC
pANCA: more commonly elevated in UC than in CD
To monitor disease activity
Fecal calprotectin and/or fecal lactoferrin: proteins associated with neutrophil activation [21]
Used as noninvasive markers of intestinal inflammation to monitor disease activity and response to therapy
Also used to differentiate IBD from irritable bowel syndrome
Inflammatory markers: CRP, ESR, platelets
CRP correlates with disease activity better than ESR; both may be normal in patients with mild CD. [11][24]
↑ Thrombocytes may be an indicator of active disease (reactive thrombocytosis) [11][25]
To identify complications
CMP: to identify malnutrition (↓ total protein), end-organ damage (↑ creatinine), and/or dehydration
CBC, iron studies, vitamin B12, folate: to evaluate for anemia and micronutrient deficiency [24]
Anemia in CD may result from chronic disease, iron deficiency, and/or vitamin B12 deficiency.
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