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Microparticles as mediators of cellular cross-talk in inflammatory disease.

机译:微粒作为炎性疾病中细胞串扰的介体。

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Microparticles are a heterogeneous population of membrane-coated vesicles which can be released from virtually all cell types during activation or apoptosis. Release occurs from the cell surface in an exogenous budding process involving local rearrangement of the cytoskeleton. Given their origin, these particles can be identified by staining for cell surface markers and annexin V. As shown in in vitro studies, microparticles may represent a novel subcellular element for intercellular communication in inflammation. Thus, microparticles can transfer chemokine receptors and arachidonic acid between cells, activate complement, promote leukocyte rolling and stimulate the release of pro-inflammatory mediators. Under certain conditions, however, microparticles may also exert anti-inflammatory properties by inducing immune cell apoptosis and the production of anti-inflammatory mediators. Microparticles may play an important role in the pathogenesis of rheumatologic diseases as evidenced by their elevation in diseases such as systemic sclerosis (SSc), systemic vasculitis and antiphospholipid antibody syndrome and correlation with clinical events. A role in inflammatory arthritis is suggested by the finding that leukocyte-derived microparticles induce the production of matrix metalloproteinases and cytokines by synovial fibroblasts. Together, these findings point to novel signaling pathways of cellular cross-talk that may operate along the spectrum of soluble cytokines and mediators of direct cell-cell contact.
机译:微粒是膜涂层囊泡的异质群体,在活化或凋亡过程中,实际上可以从所有细胞类型中释放出微粒。在涉及细胞骨架的局部重排的外源出芽过程中,从细胞表面发生释放。给定它们的来源,可以通过对细胞表面标志物和膜联蛋白V染色进行鉴定。如体外研究中所示,微粒可能代表炎症中细胞间通讯的新型亚细胞元素。因此,微粒可以在细胞之间转移趋化因子受体和花生四烯酸,激活补体,促进白细胞滚动并刺激促炎性介质的释放。然而,在某些条件下,微粒还可以通过诱导免疫细胞凋亡和产生抗炎介质来发挥抗炎特性。微粒在风湿性疾病的发病机理中可能起重要作用,这由它们在诸如系统性硬化症(SSc),系统性血管炎和抗磷脂抗体综合征等疾病中的升高以及与临床事件的相关性证明。发现白细胞衍生的微粒诱导滑膜成纤维细胞产生基质金属蛋白酶和细胞因子的发现提示了在炎性关节炎中的作用。总之,这些发现指出了细胞串扰的新信号通路,该信号通路可能沿可溶性细胞因子和直接细胞与细胞接触的介体谱起作用。

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