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Apoptosis, subcellular particles, and autoimmunity.

机译:凋亡,亚细胞颗粒和自身免疫。

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摘要

Firm evidence links the process of apoptosis to the induction of autoimmune disease. However, questions remain regarding the precise interactions of dying cells with the immune system. Genetic analyses indicate that deficiencies in serum proteins or receptors that mediate clearance of apoptotic cells increase the risk of autoimmunity. Moreover, administration of apoptotic cells to naive animals elicits transient autoimmune responses. Because known autoantigens are covalently modified and redistributed to cell surface blebs during the execution stage of apoptosis, increasing attention is being directed at this stage of programmed cell death, and researchers have identified a variety of autoantigens that are sequestered within blebs. However, blebs are merely a transition stage toward the complete cellular fragmentation, as blebs quickly convert into apoptotic bodies, subcellular particles (SCPs) of heterogeneous size, surface composition, and cargo. Because certain types of subcellular particles represent packets of highly enriched autoantigens, we propose that they are relevant to our understanding of autoimmunity.
机译:有力的证据将细胞凋亡过程与自身免疫性疾病的诱导联系起来。然而,关于垂死细胞与免疫系统的精确相互作用仍然存在疑问。遗传分析表明,介导凋亡细胞清除的血清蛋白或受体缺乏会增加自身免疫的风险。而且,向幼稚动物施用凋亡细胞会引起短暂的自身免疫反应。由于已知的自身抗原在凋亡执行阶段会被共价修饰并重新分布到细胞表面的气泡中,因此在程序性细胞死亡的这一阶段越来越引起人们的注意,研究人员已经确定了多种自身抗原被隔离在气泡中。但是,气泡只是向完整的细胞分裂的过渡阶段,因为气泡会迅速转变为凋亡小体,大小不一的表面,组成和货物的亚细胞颗粒(SCP)。由于某些类型的亚细胞颗粒代表高度富集的自身抗原,因此我们建议它们与我们对自身免疫的理解有关。

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