Author: Hedegaard, C. J.; Bendtzen, K.; Nielsen, C. H.
Title: The Role of Immune Complexes Consisting of Myelin Basic Protein (MBP), Antiâ€MBP Antibodies and Complement in Promoting CD4(+) Tâ€cell Responses to MBP in Health and Multiple Sclerosis Cord-id: r04y1j22 Document date: 2008_6_28
ID: r04y1j22
Snippet: Multiple sclerosis (MS) is an autoimmune condition characterized by degeneration of nerve fibre myelin sheets. A candidate autoantigen, myelin basic protein (MBP), has especially attracted attention. The presence of antiâ€MBP antibodies is a predictor of definite MS, but their role in the pathogenesis remains obscure. T cells have long been known to play a pivotal role in the pathogenesis of MS. Recently, an important role for B cells as autoantigenâ€presenting cells has been demonstrated in o
Document: Multiple sclerosis (MS) is an autoimmune condition characterized by degeneration of nerve fibre myelin sheets. A candidate autoantigen, myelin basic protein (MBP), has especially attracted attention. The presence of antiâ€MBP antibodies is a predictor of definite MS, but their role in the pathogenesis remains obscure. T cells have long been known to play a pivotal role in the pathogenesis of MS. Recently, an important role for B cells as autoantigenâ€presenting cells has been demonstrated in other autoimmune diseases, including rheumatoid arthritis and diabetes. The uptake of MBP by B cells and the presentation of MBPâ€derive peptides to T helper (Th) cells by B cells may be promoted by the formation of complement (C) activating immune complexes (ICs) between MBP and natural autoantibodies in healthy individuals and diseaseâ€associated antiâ€MBP antibodies in MS patients, respectively. We have investigated the formation of MBPâ€containing IC, the binding of MBP to B cells, the MBPâ€elicited induction of Thâ€cell and Bâ€cell proliferation and the cytokine production in peripheral blood mononuclear cells (PBMCs) from healthy donors grown in the presence of intact or Câ€inactivated serum from healthy donors or patients with MS. While MBP did not induce measurable proliferation of B cells nor CD4(+) T cells, we observed the production of TNFâ€Î±, IFNâ€Î³ and ILâ€10 by PBMC in response to incubation with MBP in the presence of sera from healthy controls as well as sera from MS patients. By contrast, no production of ILâ€2, ILâ€4 and ILâ€5 was detected. We are currently investigating the capability of MS sera to promote the formation of MBPâ€containing IC and thereby enhance the cytokine responses, by virtue of elevated antiâ€MBP contents.
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