â– LECTURE OVERVIEW: Granulomatous inflammation is a highly organized, chronic inflammatory response designed to wall off and contain persistent, indigestible immunogenic foreign matter.
â– THE CYTOKINE CASCADES:
1. Antigen Presentation: Macrophages phagocytose the antigen (e.g., Mycobacterium tuberculosis or sarcoidosis proteins). They process and present antigens on MHC-II molecules to CD4+ T-lymphocytes.
2. Helper T Differentiation (IL-12): Macrophages secrete Interleukin-12 (IL-12), which binds to receptors on CD4+ T cells, driving their differentiation into pro-inflammatory Th1-type helper T cells.
3. Macrophage Mobilization (IFN-Gamma): Active Th1 cells secrete Interferon-gamma (IFN-g). IFN-g is the prime macrophage activator, morphologically converting them into epithelioid histiocytes.
4. Fusion & Shells (TNF-Alpha): Under the influence of TNF-alpha, epithelioid histiocytes fuse together to form giant multinucleated Langhans-type or foreign-body giant cells, surrounded by a cuff of lymphocytes and fibroblasts.
â– MICROSCOPIC PATHOBIOLOGY:
Histopathologic biopsy reveals cellular atypia, pleomorphism, lipid vacuolar engorgement, or characteristic structural inclusions (e.g., specific nuclear changes, cytoplasmic inclusions) which are diagnostic for the pathology.
â– SUBCLINICAL PHENOTYPE DYNAMICS:
Early physiological shifts typically occur without overt symptom presentation, necessitating highly sensitive laboratory screening to detect disease onset.
[HY-BOARD-1206]
🌟 Dynamic Clinical Key:
TNF-alpha is the crucial cytokine required to preserve and maintain the integrity of a tuberculous granuloma. Chronic inflammatory arthritis patients treated with anti-TNF monoclonal antibodies (e.g., Infliximab, Adalimumab) risk rapid breakdown of these granulomatous 'shells', resulting in immediate reactivation of latent tuberculosis. Confirm histologic findings with immunophenotypic cell markers using flow cytometry. Monitor high-sensitivity panels regularly in at-risk cohorts to enable timely preventative actions.