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首页> 外文期刊>Clinical & developmental immunology. >Altered Traffic of Cardiolipin during Apoptosis: Exposure on the Cell Surface as a Trigger for 'Antiphospholipid Antibodies'
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Altered Traffic of Cardiolipin during Apoptosis: Exposure on the Cell Surface as a Trigger for 'Antiphospholipid Antibodies'

机译:细胞凋亡过程中心磷脂的改变:细胞表面的暴露作为“抗磷脂抗体”的触发条件

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Apoptosis has been reported to induce changes in the remodelling of membrane lipids; after death receptor engagement, specific changes of lipid composition occur not only at the plasma membrane, but also in intracellular membranes. This paper focuses on one important aspect of apoptotic changes in cellular lipids, namely, the redistribution of the mitochondria-specific phospholipid, cardiolipin (CL). CL predominantly resides in the inner mitochondrial membrane, even if the rapid remodelling of its acyl chains and the subsequent degradation occur in other membrane organelles. After death receptor stimulation, CL appears to concentrate into mitochondrial "raft-like" microdomains at contact sites between inner and outer mitochondrial membranes, leading to local oligomerization of proapoptotic proteins, including Bid. Clustering of Bid in CL-enriched contacts sites is interconnected with pathways of CL remodelling that intersect membrane traffic routes dependent upon actin. In addition, CL association with cytoskeleton protein vimentin was observed. Such novel association also indicated that CL molecules may be expressed at the cell surface following apoptotic stimuli. This observation adds a novel implication of biomedical relevance. The association of CL with vimentin at the cell surface may represent a "new" target antigen in the context of the apoptotic origin of anti-vimentin/CL autoantibodies in Antiphospholipid Syndrome.
机译:据报道,细胞凋亡诱导膜脂质重塑的改变。死亡受体参与后,脂质组成的特定变化不仅在质膜上发生,而且在细胞内膜上也发生。本文关注细胞脂质凋亡变化的一个重要方面,即线粒体特异性磷脂心磷脂(CL)的重新分布。 CL主要位于线粒体内膜,即使其酰基链快速重塑并随后在其他膜细胞器中降解也是如此。死亡受体刺激后,CL似乎在线粒体内外膜之间的接触点集中于线粒体“筏状”微区,导致包括Bid在内的促凋亡蛋白局部寡聚。在富含CL的接触位点中,Bid的聚类与与依赖肌动蛋白的膜运输途径相交的CL重塑途径相互关联。另外,观察到CL与细胞骨架蛋白波形蛋白相关。这种新颖的关联还表明,在凋亡刺激后,CL分子可能在细胞表面表达。该观察结果增加了生物医学相关性的新颖含义。在抗磷脂综合症中抗波形蛋白/ CL自身抗体的凋亡起源的背景下,CL与波形蛋白在细胞表面的缔合可能代表“新的”靶抗原。

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