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IM30/Vipp1 羧基端与脂双层结合并调节膜融合。

The IM30/Vipp1 C-terminus associates with the lipid bilayer and modulates membrane fusion.

机构信息

Institut für Pharmazie und Biochemie, Johannes Gutenberg-Universität Mainz, 55128 Mainz, Germany.

Department of Biomedical Engineering, University of Minnesota, Twin Cities, MN, USA.

出版信息

Biochim Biophys Acta Bioenerg. 2017 Feb;1858(2):126-136. doi: 10.1016/j.bbabio.2016.11.004. Epub 2016 Nov 9.

Abstract

IM30/Vipp1 proteins are crucial for thylakoid membrane biogenesis in chloroplasts and cyanobacteria. A characteristic C-terminal extension distinguishes these proteins from the homologous bacterial PspA proteins, and this extension has been discussed to be key for the IM30/Vipp1 activity. Here we report that the extension of the Synechocystis IM30 protein is indispensable, and argue that both, the N-terminal PspA-domain as well as the C-terminal extension are needed in order for the IM30 protein to conduct its in vivo function. In vitro, we show that the PspA-domain of IM30 is vital for stability/folding and oligomer formation of IM30 as well as for IM30-triggered membrane fusion. In contrast, the IM30 C-terminal domain is involved in and necessary to stabilize defined contacts to negatively charged membrane surfaces, and to modulate the IM30-induced membrane fusion activity. Although the two IM30 protein domains have distinct functional roles, only together they enable IM30 to work properly.

摘要

IM30/Vipp1 蛋白对于叶绿体和蓝藻中的类囊体膜生物发生至关重要。它们的 C 末端特征延伸区分了这些蛋白与同源的细菌 PspA 蛋白,并且这个延伸被认为是 IM30/Vipp1 活性的关键。在这里,我们报告说,Synechocystis 的 IM30 蛋白的延伸是必不可少的,并认为 N 端的 PspA 结构域和 C 端的延伸对于 IM30 蛋白执行其体内功能都是必需的。在体外,我们表明 IM30 的 PspA 结构域对于 IM30 的稳定性/折叠和寡聚形成以及 IM30 触发的膜融合都是至关重要的。相比之下,IM30 的 C 末端结构域参与并需要稳定与带负电荷的膜表面的特定接触,并调节 IM30 诱导的膜融合活性。尽管这两个 IM30 蛋白结构域具有不同的功能作用,但只有它们共同作用才能使 IM30 正常工作。

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