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Inflammatory Bowel Disease

Inflammatory Bowel Disease. A Aljebreen , MD, FRCPC Jan 2010. Objectives. Introduction Classifications Clinical features Diagnosis Management Conclusion. Introduction.

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Inflammatory Bowel Disease

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  1. Inflammatory Bowel Disease A Aljebreen, MD, FRCPC Jan 2010

  2. Objectives Introduction Classifications Clinical features Diagnosis Management Conclusion

  3. Introduction • IBD characterized by a tendency for chronic or relapsing immune activation and inflammation within the gastrointestinal tract (GIT) • Crohn’s disease (CD) and ulcerative colitis (UC) are the 2 major forms of idiopathic IBD.

  4. Less common entities • Microscopic colitis (collagenous and lynphocytic) • Others • Diversion colitis • Radiation colitis • Drug induced colitis • Infectious colitis • Ischemic colitis

  5. CD and UC • CD is a condition of • Chronic inflammation potentially involving any location of the GIT from mouth to anus. • It is a lifelong disease arising from an interaction between genetic and environmental factors • UC is an inflammatory disorder that affects the rectum and extends proximally to affect variable extent of the colon.

  6. Epidemiology • CD: • 1st peak 15-30 years of age, 2nd peak around 60 y • There is a definite incidence surge in Saudi Arabia over the last 10 years • UC: • High incidence areas: US, UK, northern Europe • Young adults, commoner in females

  7. Genetics • Studies suggested that 1st degree relatives of an affected patient have a risk of IBD that is 4-20 times higher than that of general population. • The best replicated linkage region, IBD1, on chromosome 16q contains the CD susceptibility gene, NOD2/CARD15. • Having one copy of the risk alleles confers a 2–4-fold risk for developing CD, whereas double-dose carriage increases the risk 20–40-fold.

  8. Etiology • Mutations within the NOD2/ CARD15 gene contribute to CD susceptibility. • Functional studies suggest that inappropriate responses to bacterial components may alter signaling pathways of the innate immune system, leading to • the development and persistence of intestinal inflammation. • Initiating pathogen? • Infectious? • ? Possibly non-pathogenic commensal enteric flora

  9. Pathogenesis • The mucosa of CD patients is dominated by Th1 (T helper), which produce interferon-γ and IL-2. • In contrast, UC dominated by Th2 phenotype, which produce transforming growth factor (TGF-) and IL-5. • Activation of Th1 cells produce the down-regulatory cytokines IL-10 and TGF-.

  10. Environmental Precipitants • Factors: • NSAIDs use (?altered intestinal barrier), and • Early appendectomy (increase UC incidence) • Smoking (protects against UC but increases the risk of CD).

  11. CD: PATHOLOGY • Early Findings: • Aphthous ulcer. • The presence of granulomas • Late findings: • Linear ulcers. • The classic cobble stoned appearance may arise. • Transmural inflammation • Sinus tracts, and strictures. • Fibrosis.

  12. transmural inflammation with predominance of the inflammation in the mucosa and submucosa.

  13. UC: PATHOLOGY • The inflammation is predominantly confined to the mucosa. • Non-specific (can be seen with any acute inflammation) • The lamina propria becomes edematous. • Inflammatory infiltrate of neutrophils • Neutrophils invade crypts, causing cryptitis & ultimately crypt abscesses. • Specific (suggest chronicity): • Distorted crypt architecture, crypt atrophy and a chronic inflammatory infiltrate.

  14. Diagnosis • Exclude other possibilities (need good history, physical exam, labs, imaging and endoscopy with biopsy) • There are many distinguishing features of CD and UC. • In about 5% it is classified as indeterminate because of overlapping features.

  15. Distinguishing characteristics of CD and UC

  16. Endoscopic features of CD and UC

  17. Pathologic features of CD and UC

  18. Radiologic features of CD and UC

  19. UC: Presentation • Must exclude infectious cause before making Dx. • Rectal Bleeding • Diarrhea: • frequent passage of loose or liquid stool, often associated with passing large quantities of mucus. • Abdominal Pain: • it is not a prominent symptom. • Anorexia, nausea, fever…

  20. DDX of UC • Infectious • Drug induced • Microscopic colitis

  21. UC: Presentation • Mild attack: • Most common form, mainly left sided colitis, <4 BM/day with no blood • Moderate attack: • 25% of all patients, 4-6 BM/day with blood. • Severe or fulminant colitis: • ~ 15% of cases, >6BM/day, bloody, fever, weight loss, diffuse abd tenderness, elevated WBC, most refractory to medical therapy

  22. CD • Anatomic distribution • CD activity index • DDx (lymphoma, Yersinea Enterocolitis, TB)

  23. CD: clinical presentations • Disease of the ileum: • May present initially with a small bowel obstruction. • Patients with an active disease often present with anorexia, loose stools, and weight loss. • Perianal disease • In 24% of patients with CD. • Skin lesions include superficial ulcers, and abscesses. • Anal canal lesions include fissures, ulcers, and stenosis.

  24. CD ilitis: DDx • Lymphoma • Yersinea Enterocolitis and • TB

  25. CD: clinical presentations • colonic disease • The typical presenting symptom is diarrhea, occasionally with passage of obvious blood. • proctitis • May be the initial presentation in some cases of CD

  26. Extra-intestinal manifestations of IBD • Arthritis: • Peripheral arthritis, usu paralels the disease activity • Ankylosing Spondylitis, 1-6%, sacroiliitis • Ocular lesions: • Iritis (uvietis) (0.5-3%), episcleritis, keratitis, • Skin and oral cavity: • Erythema nodosum 1-3% • Pyoderma Gangrenosum 0.6% • Aphthus stomatitis, metastatic CD.

  27. Extra-intestinal manifestations of IBD • Liver and Biliary tract disease: • Pericholangitis, fatty infiltration, PSC (1-4%, more with UC), cholangiocarcinoma, gallstones • Thromboembolic disease, vasculitis, Renal disease (urolithiasis, GN), clubbing, amyloidosis.

  28. Complications of IBD • Bleeding • Stricture • Fistula • Toxic megacolon • Cancer

  29. How to diagnose IBD • History • Physical examinations • Labs • Radiology • Endoscopy • Histopathology

  30. Case scenario 1 • 17 year old female presented with 1 year history of intermittent abdominal cramps and increasing abdominal gases and bloating. • What other history you want?

  31. Case scenario 2 • 65 year old male presented with 6 months history of bleeding per rectum. • What other history you want? • What else you need?

  32. Treatment • Goals of therapy • Induce and maintain remission. • Ameliorate symptoms • Improve pts quality of life • Adequate nutrition • Prevent complication of both the disease and medications

  33. 5-Aminosalicylic Acids • The mainstay treatment of mild to moderately active UC and CD (induction). • 5-ASA may act by • blocking the production of prostaglandins and leukotrienes, • inhibiting bacterial peptide–induced neutrophil chemotaxis and adenosine-induced secretion, • scavenging reactive oxygen metabolites

  34. 5-Aminosalicylic Acids • For patients with distal colonic disease, a suppository or enema form will be most appropriate. • Maintenance treatment with a 5-aminosalicylic acid can be effective for sustaining remission in ulcerative colitis but is of questionable value in Crohn's disease.

  35. Corticosteroids • Topical corticosteroids can be used as an alternative to 5-ASA in ulcerative proctitis or distal UC. • Oral prednisone or prednisolone is used for moderately severe UC or CD, in doses ranging up to 60 mg per day. • IV is warranted for patients who are sufficiently ill to require hospitalization; the majority will have a response within 7 to 10 days.

  36. Corticosteroids • No proven maintenance benefit in the treatment of either UC or CD. • Many and serious side effects. • Budesonide: • less side effects, • its use is limited to patients with distal ileal and right-sided colonic disease

  37. Immunosuppressive Agents • These agents are generally appropriate for patients in whom the dose of corticosteroids cannot be tapered or discontinued. • Azathioprine & 6-MP • The most extensively used immunosuppressive agents. • The mechanisms of action unknown but may include • suppressing the generation of a specific subgroup of T cells. • The onset of benefit takes several weeks up to six months. • Dose-related BM suppression is uniformly observed

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