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Phosphatidylserine, a death knell.

机译:磷脂酰丝氨酸,丧钟。

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Virtually every cell in the body restricts phosphatidylserine (PS) to the inner leaflet of the plasma membrane by energy-dependent transport from the outer to the inner leaflet of the bilayer. Apoptotic cells of all types rapidly randomize the asymmetric distribution, bringing PS to the surface where it serves as a signal for phagocytosis. A myriad of phagocyte receptors have been implicated in the recognition of apoptotic cells, among them a PS receptor, yet few ligands other than PS have been identified on the apoptotic cell surface. Since apoptosis and the associated exposure of PS on the cell surface is probably over 600 million years old, it is not surprising that evolution has appropriated aspects of this process for specialized purposes such as blood coagulation, membrane fusion and erythrocyte differentiation. Failure to efficiently remove apoptotic cells may contribute to inflammatory responses and autoimmune diseases resulting from chronic, inappropriate exposure of PS.
机译:实际上,体内的每个细胞都通过从双层的外部小叶到内部小叶的能量依赖性转运,将磷脂酰丝氨酸(PS)限制在质膜的内部小叶。各种类型的凋亡细胞迅速使不对称分布随机化,使PS到达表面,成为吞噬信号。已经有无数的吞噬细胞受体参与凋亡细胞的识别,其中包括PS受体,但在凋亡细胞表面上除了PS以外几乎没有发现任何配体。由于细胞凋亡和相关的PS在细胞表面的暴露可能已经超过6亿年了,因此进化将这一过程的各个方面用于特殊目的(例如凝血,膜融合和红细胞分化)并不奇怪。无法有效清除凋亡细胞可能是由于长期,不适当暴露于PS导致的炎症反应和自身免疫性疾病。

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