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From the Cover: Structural basis for membrane targeting by the MVB12-associated β-prism domain of the human ESCRT-I MVB12 subunit

机译:从封面开始:人ESCRT-1 MVB12亚基与MVB12相关的β-棱镜域靶向膜的结构基础

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摘要

MVB12-associated β-prism (MABP) domains are predicted to occur in a diverse set of membrane-associated bacterial and eukaryotic proteins, but their existence, structure, and biochemical properties have not been characterized experimentally. Here, we find that the MABP domains of the MVB12A and B subunits of ESCRT-I are functional modules that bind in vitro to liposomes containing acidic lipids depending on negative charge density. The MABP domain is capable of autonomously localizing to subcellular puncta and to the plasma membrane. The 1.3-Å atomic resolution crystal structure of the MVB12B MABP domain reveals a β-prism fold, a hydrophobic membrane-anchoring loop, and an electropositive phosphoinositide-binding patch. The basic patch is open, which explains how it senses negative charge density but lacks stereoselectivity. These observations show how ESCRT-I could act as a coincidence detector for acidic phospholipids and protein ligands, enabling it to function both in protein transport at endosomes and in cytokinesis and viral budding at the plasma membrane.
机译:MVB12相关的β-棱镜(MABP)域预计会发生在各种与膜相关的细菌和真核蛋白质中,但是它们的存在,结构和生化特性尚未通过实验表征。在这里,我们发现ESCRT-1的MVB12A和B亚基的MABP结构域是功能模块,可根据负电荷密度在体外与含有酸性脂质的脂质体结合。 MABP结构域能够自主定位于亚细胞点和质膜。 MVB12B MABP结构域的1.3-Å原子分辨率晶体结构显示β棱镜折叠,疏水性膜锚定环和正电磷酸肌醇结合斑块。基本的贴片是开放的,这说明了它如何感测负电荷密度,但缺乏立体选择性。这些观察结果表明,ESCRT-1可以充当酸性磷脂和蛋白质配体的同时检测器,从而使其在核糖体的蛋白转运,胞质分裂和质膜的病毒萌芽中发挥作用。

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