首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >Schwann cells and myasthenia gravis. Preferential uptake of soluble and membrane-bound AChR by normal and immortalized Schwann cells and immunogenic presentation to AChR-specific T line lymphocytes.
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Schwann cells and myasthenia gravis. Preferential uptake of soluble and membrane-bound AChR by normal and immortalized Schwann cells and immunogenic presentation to AChR-specific T line lymphocytes.

机译:雪旺氏细胞和重症肌无力。正常和永生化的施万细胞优先吸收可溶性和膜结合的AChR并向AChR特异性T线淋巴细胞免疫原性呈递。

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摘要

The normal neuromuscular synapse is formed by the intimate association of nerve endings, postsynaptic end-plate foldings in the muscle fiber, and nonmyelinating Schwann cells (SC) sealing the synaptic ramifications. Because SC have been recognized recently to have an immunogenic potential inducible to present protein autoantigens to autoimmune T lymphocytes, and considering their close proximity to the acetylcholine receptor (AChR)-bearing postsynaptic membranes, presentation of soluble and membrane vesicle-bound AChR to appropriate T cells was investigated. Short-term monolayer cultures of SC isolated from neonatal rat sciatic nerves, as well as cells of an immortalized SC line of similar origin, were fully able to present the relevant molecular epitopes to major histocompatibility complex (MHC) compatible AChR-specific T line lymphocytes immunogenically. Presentation of AChR was restricted by RT1.B (I-A) MHC class II products. Both types of cultured rat SC were inducible to expression of MHC class I and II products, and they were able to phagocytose AChR-enriched membrane vesicles preferentially. In contrast, phagocytosis of latex particles by SC was negligible. These data qualify perisynaptic SC as potential presenter cells of autoimmunogenic AChR in myasthenia gravis. Thus, SC may play a critical and as-yet unpredicted regulatory role in the cellular pathogenesis of myasthenia gravis.
机译:正常的神经肌肉突触是由神经末梢,肌肉纤维中的突触后终板折叠和密封突触分支的无髓鞘雪旺细胞(SC)紧密相关而形成的。因为最近已经认识到SC具有可诱导的蛋白原抗原向自身免疫T淋巴细胞呈递的免疫原性潜力,并考虑到它们与带有乙酰胆碱受体(AChR)的突触后膜非常接近,所以将可溶性和膜囊泡结合的AChR呈递给合适的T细胞进行了调查。从新生大鼠坐骨神经分离的SC的短期单层培养以及具有相似来源的永生化SC系的细胞完全能够向主要组织相容性复合物(MHC)兼容的AChR特异性T系淋巴细胞呈递相关的分子表位免疫原性的。 RT1.B(I-A)MHC II类产品限制了AChR的表达。两种类型的培养的大鼠SC均可诱导表达MHC I和II类产物,并且它们能够优先吞噬富含AChR的膜囊泡。相反,SC对乳胶颗粒的吞噬作用可忽略不计。这些数据使突触周围SC成为重症肌无力中自身免疫原性AChR的潜在呈递细胞。因此,SC可能在重症肌无力的细胞发病机理中起着至关重要的和尚未预测的调节作用。

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