首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Dual implication of 23-cyclic nucleotide 3 phosphodiesterase as major autoantigen and C3 complement-binding protein in the pathogenesis of multiple sclerosis.
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Dual implication of 23-cyclic nucleotide 3 phosphodiesterase as major autoantigen and C3 complement-binding protein in the pathogenesis of multiple sclerosis.

机译:23-环核苷酸3磷酸二酯酶作为多发性硬化症发病机理中的主要自身抗原和C3补体结合蛋白的双重含义。

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摘要

Multiple sclerosis (MS) is characterized by intra-blood-brain barrier immunoglobulin synthesis that persists lifelong. Subcellular fractionation and two-dimensional electrophoresis were used in conjunction with immune precipitation and immunoblotting to identify antigenic determinants for this immunoglobulin. We report that 2', 3'-cyclic nucleotide 3'-phosphodiesterase (CNP), a protein associated with oligodendrocyte/myelin membranes, also present in lymphocytes and retina, is one major target for the humoral response. Antibodies to CNP are detected in sera of 74% of MS patients. The antibodies are IgM and are present in serum in high titer as well as in cerebrospinal fluid. The antibody response is temporally persistent, consistent with systemic immune activation and persistent antigenic stimulation. Moreover, CNP is isolated as an immune complex from MS brain. CNP is expressed as two isoforms, with CNPII identical to CNPI but with a 20-amino acid extension at the amino terminus of CNPII; however, the antibody response is exclusively restricted to CNPI. In contrast, both isoforms bind the C3 complement, providing a plausible mechanism in MS central nervous system (CNS) for opsonization of myelin membrane CNP, mediated via the C3 receptor, and phagocytosis of CNP-Ig immune complexes, mediated by membrane Ig Fc receptors of macrophages and CNS microglia.
机译:多发性硬化症(MS)的特征是血脑屏障内免疫球蛋白的合成持续一生。亚细胞分级分离和二维电泳与免疫沉淀和免疫印迹结合使用,以鉴定该免疫球蛋白的抗原决定簇。我们报告说2',3'-环核苷酸3'-磷酸二酯酶(CNP),与少突胶质细胞/髓鞘膜相关的蛋白质,也存在于淋巴细胞和视网膜中,是体液反应的主要目标。在74%的MS患者血清中检测到CNP抗体。抗体是IgM,以高滴度存在于血清以及脑脊髓液中。抗体反应是暂时性的,与全身性免疫激活和持续性抗原刺激相一致。此外,CNP是作为免疫复合物从MS脑中分离出来的。 CNP被表示为两个同工型,其中CNPII与CNPI相同,但在CNPII的氨基末端具有20个氨基酸的延伸;但是,抗体反应仅限于CNPI。相反,两种同工型均结合C3补体,从而在MS中枢神经系统(CNS)中为通过C3受体介导的髓磷脂膜CNP调理和由膜Ig Fc受体介导的CNP-Ig免疫复合物的吞噬作用提供了合理的机制。巨噬细胞和中枢神经系统小胶质细胞。

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