Inflammatory Bowel Disease (IBD)
Inflammatory Bowel Disease (IBD) is a chronic immune-mediated inflammatory disorder of the gastrointestinal tract.
Major subtypes:
- Crohn Disease
- Ulcerative Colitis
IBD is characterized by inappropriate immune activation against intestinal microbiota in genetically susceptible individuals.
Core Pathophysiology
IBD results from:
- Disrupted epithelial barrier function
- Dysregulated innate immunity
- Pathologic T-cell activation
- Cytokine-driven inflammation
Central inflammatory mediators:
- TNF-α
- IL-12
- IL-23
- IL-17
- IL-13 (more prominent in UC)
Chronic inflammation leads to:
- Ulceration
- Edema
- Fibrosis (Crohn)
- Continuous mucosal injury (UC)
Immunologic Distinction: Crohn vs Ulcerative Colitis
Although both are immune-mediated diseases, the dominant pathways differ.
Crohn Disease – Th1 / Th17 Dominant
Primary drivers:
- Th1 cells
- Th17 cells
Key cytokines:
- TNF-α
- IFN-γ
- IL-12
- IL-23
- IL-17
Mechanism:
IL-12 and IL-23 promote Th1/Th17 differentiation → Macrophage and neutrophil recruitment → Transmural inflammation.
Clinical consequences:
- Fistulas
- Abscesses
- Strictures
- Deep ulceration
Therapeutic targets:
Ulcerative Colitis – Th2-Like Cytokine Pattern
Primary features:
- Th2-like immune activation
- IL-5 and IL-13 predominance
Key cytokines:
- IL-13
- IL-5
- TNF-α
Mechanism:
IL-13-mediated epithelial injury → Barrier dysfunction → Superficial mucosal inflammation.
Clinical consequences:
- Continuous lesions
- Mucosal-only disease
- Bloody diarrhea
Therapeutic targets:
- Anti-TNF agents
- Vedolizumab (gut-selective)
Crohn vs Ulcerative Colitis Comparison
| Feature | Crohn Disease | Ulcerative Colitis |
|---|---|---|
| Location | Anywhere mouth → anus | Colon only |
| Pattern | Skip lesions | Continuous |
| Depth | Transmural | Mucosal only |
| Fistulas | Common | Rare |
| Strictures | Common | Rare |
| Bloody diarrhea | Less common | Common |
| Cancer risk | Increased | Increased (higher with duration) |
Clinical Presentation
Common symptoms:
- Chronic diarrhea
- Abdominal pain
- Weight loss
- Fatigue
Crohn-specific:
- Perianal disease
- Fistulas
- Obstruction
UC-specific:
- Bloody diarrhea
- Tenesmus
Extraintestinal manifestations:
- Arthritis
- Uveitis
- Erythema nodosum
- Primary sclerosing cholangitis
Treatment Strategy
Goals:
- Induce remission
- Maintain remission
- Prevent complications
- Minimize steroid exposure
Therapy depends on disease severity and phenotype.
Pharmacologic Management
1. Mild Disease (Primarily Ulcerative Colitis)
Aminosalicylates:
Mechanism:
Local suppression of prostaglandins and leukotrienes in colonic mucosa.
Limited efficacy in Crohn disease.
2. Induction Therapy (Moderate–Severe Flares)
Corticosteroids:
- Budesonide (GI-targeted)
Mechanism:
Broad suppression of cytokine transcription.
Not used for maintenance due to:
- HPA axis suppression
- Osteoporosis
- Infection risk
See:
3. Maintenance Therapy
Immunomodulators:
Mechanism:
Suppress lymphocyte proliferation.
Used as:
- Steroid-sparing agents
- Maintenance therapy
4. Biologic Therapy (Moderate–Severe Disease)
Anti-TNF agents:
Anti-IL-12/23:
Anti-integrin (gut selective):
Mechanisms:
- TNF blockade reduces inflammatory cascade.
- IL-12/23 blockade suppresses Th1/Th17 differentiation.
- Integrin blockade prevents leukocyte trafficking to gut.
Complications
Crohn:
- Fistulas
- Abscesses
- Obstruction
- Malnutrition
Ulcerative Colitis:
- Toxic megacolon
- Severe hemorrhage
- Colorectal cancer (long-standing disease)
Both:
- Anemia
- Thromboembolism
- Osteoporosis (steroid-related)
High-Yield Pearls
- Crohn = Th1/Th17 dominant → transmural inflammation.
- UC = Th2-like cytokine pattern → mucosal-only disease.
- TNF-α is central in both diseases.
- Steroids induce remission but do not maintain it.
- IL-12/23 pathway is especially important in Crohn.
- Long-standing UC increases colorectal cancer risk.