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Mammalian GPI-anchored proteins require p24 proteins for their efficient transport from the ER to the plasma membrane

机译:哺乳动物GPI锚定蛋白需要p24蛋白才能有效地从ER转运到质膜

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pThe GPI (glycosylphosphatidylinositol) moiety is attached to newly synthesized proteins in the lumen of the ER (endoplasmic reticulum). The modified proteins are then directed to the PM (plasma membrane). Less well understood is how nascent mammalian GPI-anchored proteins are targeted from the ER to the PM. In the present study, we investigated mechanisms underlying membrane trafficking of the GPI-anchored proteins, focusing on the early secretory pathway. We first established a cell line that stably expresses inducible temperature-sensitive GPI-fused proteins as a reporter and examined roles of transport-vesicle constituents called p24 proteins in the traffic of the GPI-anchored proteins. We selectively suppressed one of the p24 proteins, namely p23, employing RNAi (RNA interference) techniques. The suppression resulted in pronounced delays of PM expression of the GPI-fused reporter proteins. Furthermore, maturation of DAF (decay-accelerating factor), one of the GPI-anchored proteins in mammals, was slowed by the suppression of p23, indicating delayed trafficking of DAF from the ER to the Golgi. Trafficking of non-GPI-linked cargo proteins was barely affected by p23 knockdown. This is the first to demonstrate direct evidence for the transport of mammalian GPI-anchored proteins being mediated by p24 proteins./p
机译:> GPI(糖基磷脂酰肌醇)部分在ER(内质网)内腔中与新合成的蛋白质连接。然后将修饰的蛋白质导向PM(质膜)。鲜为人知的是如何将新生的哺乳动物GPI锚定蛋白质从ER靶向到PM。在本研究中,我们调查了GPI锚定蛋白质的膜运输的机制,重点是早期分泌途径。我们首先建立了一种稳定地表达可诱导温度敏感的GPI融合蛋白作为报告基因的细胞系,并研究了称为p24蛋白的运输囊泡成分在GPI锚定蛋白的运输中的作用。我们使用RNAi(RNA干扰)技术选择性抑制p24蛋白之一,即p23。该抑制导致GPI融合的报道蛋白的PM表达的明显延迟。此外,哺乳动物中GPI固定蛋白之一DAF(衰变促进因子)的成熟由于抑制p23而减慢,表明DAF从ER到高尔基体的运输被延迟。非GPI连接的货物蛋白的贩运几乎不受p23敲低的影响。这是第一个直接证明由p24蛋白介导的哺乳动物GPI锚定蛋白转运的证据。

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