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Differential effect of phosphatidylethanolamine depletion on raft proteins - Further evidence for diversity of rafts in Saccharomyces cerevisiae

机译:磷脂酰乙醇胺消耗对木筏蛋白质的差异影响-酿酒酵母中木筏多样性的进一步证据

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摘要

A considerable amount of evidence supports the idea that lipid rafts are involved in many cellular processes, including protein sorting and trafficking. We show that, in this process, also a non-raft lipid, phosphatidylethanolamine (PE), has an indispensable function. The depletion of this phospholipid results in an accumulation of a typical raft-resident, the arginine transporter Can I p, in the membranes of Golgi, while the trafficking of another plasma membrane transporter, Pma1p, is interrupted at the level of the ER. Both these transporters associate with a Triton (TX-100) resistant membrane fraction before their intracellular transport is arrested in the respective organelles. The Can1p undelivered to the plasma membrane is fully active when reconstituted to a PE-containing vesicle system in vitro. We further demonstrate that, in addition to the TX-100 resistance at 4 degrees C, Can I p and Pma1pa exhibit different accessibility to nonyl glucoside (NG), which points to distinct intimate lipid surroundings of these two proteins. Also, at 20 degrees C, these two proteins are extracted by TX-100 differentially. The features above suggest that Pma1p and Can1p are associated with different compartments. This is independently supported by the observations made by confocal microscopy. In addition we show that PE is involved in the stability of Can1p-raft association. (c) 2005 Elsevier B.V All rights reserved.
机译:大量证据支持脂质筏参与许多细胞过程的想法,包括蛋白质分选和运输。我们显示,在此过程中,非漂流脂质磷脂酰乙醇胺(PE)也具有必不可少的功能。这种磷脂的消耗导致高尔基体膜中典型的筏驻留精氨酸转运蛋白Can I p的积累,而另一种质膜转运蛋白Pma1p的转运在ER水平被中断。这两种转运蛋白均与Triton(TX-100)抗性膜部分相关,然后将它们的细胞内转运阻滞在各个细胞器中。当体外重构为含PE的囊泡系统时,未传递至质膜的Can1p具有完全活性。我们进一步证明,除了在4摄氏度下的TX-100抗性外,Can I p和Pma1pa还具有对壬基糖苷(NG)的不同可及性,这表明这两种蛋白质具有独特的亲密脂质环境。同样,在20摄氏度下,这两种蛋白质被TX-100差异提取。上面的功能表明Pma1p和Can1p与不同的隔离专区相关联。共聚焦显微镜的观察结果独立地支持了这一点。此外,我们证明了PE参与Can1p-raft关联的稳定性。 (c)2005 Elsevier B.V保留所有权利。

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