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l�ll B cells as under-appreciated mediators of non-auto-immune inflammatory disease Nikolajczyk BSCytokine 2010[Jun]; 50 (3): 234-42B lymphocytes play roles in many auto-immune diseases characterized by unresolved inflammation, and B cell ablation is proving to be a relatively safe, effective treatment for such diseases. B cells function, in part, as important sources of regulatory cytokines in auto-immune disease, but B cell cytokines also play roles in other non-auto-immune inflammatory diseases. B cell ablation may therefore benefit inflammatory disease patients in addition to its demonstrated efficacy in auto-immune disease. Current ablation drugs clear both pro- and anti-inflammatory B cell subsets, which may unexpectedly exacerbate some pathologies. This possibility argues that a more thorough understanding of B cell function in human inflammatory disease is required to safely harness the clinical promise of B cell ablation. Type 2 diabetes (T2D) and periodontal disease (PD) are two inflammatory diseases characterized by little autoimmunity. These diseases are linked by coincident presentation and alterations in toll-like receptor (TLR)-dependent B cell cytokine production, which may identify B cell ablation as a new therapy for co-affected individuals. Further analysis of the role B cells and B cell cytokines play in T2D, PD and other inflammatory diseases is required to justify testing B cell depletion therapies on a broader range of patients.|Autoimmunity/immunology[MESH]|B-Lymphocytes/*immunology/*pathology[MESH]|Cytokines/immunology[MESH]|Diabetes Mellitus, Type 2/immunology[MESH]|Humans[MESH]|Inflammation/immunology/*pathology[MESH]|Periodontal Diseases/immunology[MESH] |