首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Insig-2, a second endoplasmic reticulum protein that binds SCAP and blocks export of sterol regulatory element-binding proteins
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Insig-2, a second endoplasmic reticulum protein that binds SCAP and blocks export of sterol regulatory element-binding proteins

机译:Insig-2,第二种内质网蛋白,与SCAP结合并阻止固醇调节元件结合蛋白的输出

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This paper describes insig-2, a second protein of the endoplasmic reticulum that blocks the processing of sterol regulatory element-binding proteins (SREBPs) by binding to SCAP (SREBP cleavage-activating protein) in a sterol-regulated fashion, thus preventing it from escorting SREBPs to the Golgi. By blocking this movement, insig-2, like the previously described insig-1, prevents the proteolytic processing of SREBPs by Golgi enzymes, thereby blacking cholesterol synthesis. The sequences of human insig-1 and -2 are 59% identical. Both proteins are predicted to contain six transmembrane helices. The proteins differ functionally in two respects: (ⅰ) production of insig-1, but not insig-2, in cultured mammalian cells requires nuclear SREBPs; and (ⅱ) at high levels of expression, insig-1, but not insig-2, can block SCAP movement in the absence of exogenous sterols. The combined actions of insig-1 and -2 permit feedback regulation of cholesterol synthesis over a wide range of sterol concentrations.
机译:本文介绍了insig-2,这是内质网的第二种蛋白,它通过以固醇调节的方式与SCAP(SREBP裂解激活蛋白)结合来阻止固醇调节元件结合蛋白(SREBPs)的加工。护送SREBP到高尔基体。通过阻止这种运动,insig-2就像之前的insig-1一样,阻止了高尔基酶对SREBP的蛋白水解过程,从而使胆固醇合成变黑。人类insig-1和-2的序列相同,相差59%。预测这两种蛋白质均包含六个跨膜螺旋。蛋白质在两个方面在功能上有所不同:(ⅰ)在培养的哺乳动物细胞中产生insig-1,而不产生insig-2,需要核SREBP。 (ⅱ)高表达水平,insig-1(而不是insig-2)可以在没有外源固醇的情况下阻止SCAP的运动。 insig-1和-2的共同作用允许在很宽的固醇浓度范围内进行胆固醇合成的反馈调节。

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