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首页> 外文期刊>Biochemical Pharmacology >Regulation of phosphatidylserine exposure at the cell surface by the serine--base exchange enzyme system during CD95-induced apoptosis.
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Regulation of phosphatidylserine exposure at the cell surface by the serine--base exchange enzyme system during CD95-induced apoptosis.

机译:在CD95诱导的细胞凋亡过程中,丝氨酸-碱基交换酶系统调节磷脂酰丝氨酸在细胞表面的暴露。

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摘要

Early in the apoptotic process, CD95 induces a translocation of phosphatidylserine (PtdSer) from the inner to the outer leaflet of the cellular plasma membrane. In mammalian cells, PtdSer is only synthesized through a calcium-dependent exchange of the polar head group of pre-existing phospholipids, either phosphatidylcholine or phosphatidylethanolamine, by a serine. Using a pharmacological approach, we examined the influence of PtdSer synthesis on CD95-induced PtdSer exposure at the surface of Jurkat cells. We found that CD3/TCR triggering or thapsigargin treatment of Jurkat cells was accompanied both by a decreased PtdSer synthesis and by a strong reduction of CD95-induced PtdSer at the cell surface, as monitored by fluorescence-activated cell sorting (FACS) analysis of annexin V-fluorescein isothiocyanate (FITC)-labeled cells. PtdSer synthesis through the serine-base exchange enzyme system thus appeared as one of the mechanisms implicated in the recently discovered CD3/TCR-induced down-regulation of CD95-induced apoptosis. Conversely, increasing the activity of the serine-base exchange enzyme system with different drugs, either the K+ channel blocker quinine, the cationic amphiphil stearylamine, or three different calmodulin antagonists, chlorpromazine, trifluoperazine, and N-(6-aminohexyl)-5-chloro-1-naphthalene sulfonamide (W7), resulted in an increased appearance of PtdSer at the surface of CD95-treated cells. Both PtdSer synthesis and CD95-induced annexin V-FITC reactivity were abrogated in ATP-depleted cells. Also, modifying the membrane potential with valinomycin (hyperpolarization) or either gramicidin or KCl (depolarization) demonstrated a strong relationship between PtdSer synthesis and annexin V-FITC reactivity in CD95-treated cells. Together, our results indicate that CD95-induced exposure of PtdSer at the cell surface could be regulated by the activity of the serine-base exchange enzyme system.
机译:在凋亡过程的早期,CD95诱导磷脂酰丝氨酸(PtdSer)从细胞质膜的内小叶向外小叶易位。在哺乳动物细胞中,PtdSer仅通过丝氨酸通过钙依赖性交换预先存在的磷脂(磷脂酰胆碱或磷脂酰乙醇胺)的极性头部基团来合成。使用药理学方法,我们检查了PtdSer合成对Jurkat细胞表面CD95诱导的PtdSer暴露的影响。我们发现,如膜联蛋白的荧光激活细胞分选(FACS)分析所监测,Jurkat细胞的CD3 / TCR触发或毒胡萝卜素处理伴随着PtdSer合成的减少和CD95诱导的PtdSer在细胞表面的强烈减少。 V-荧光素异硫氰酸酯(FITC)标记的细胞。因此,通过丝氨酸碱基交换酶系统合成PtdSer成为最近发现的CD3 / TCR诱导的CD95诱导的细胞凋亡下调的机制之一。相反,使用不同的药物(K +通道阻滞剂奎宁,阳离子两亲硬脂胺或三种不同的钙调蛋白拮抗剂,氯丙嗪,三氟哌嗪和N-(6-氨基己基)-5-)增加丝氨酸碱基交换酶系统的活性。氯-1-萘磺酰胺(W7)在CD95处理的细胞表面导致PtdSer的外观增加。在ATP耗尽的细胞中,PtdSer合成和CD95诱导的膜联蛋白V-FITC反应性均被废除。同样,用缬氨霉素(超极化)或短杆菌肽或KCl(去极化)修饰膜电位表明,在CD95处理的细胞中PtdSer合成与膜联蛋白V-FITC反应性之间存在很强的关系。总之,我们的结果表明CD95诱导的PtdSer在细胞表面的暴露可以通过丝氨酸碱基交换酶系统的活性来调节。

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