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Bax-α1靶向序列如何与线粒体膜相互作用?心磷脂的作用。

How does the Bax-alpha1 targeting sequence interact with mitochondrial membranes? The role of cardiolipin.

作者信息

Sani Marc-Antoine, Dufourc Erick J, Gröbner Gerhard

机构信息

UMR 5248 CBMN, CNRS, Université Bordeaux 1, ENITAB, IECB, 33607 Pessac Cedex, France.

出版信息

Biochim Biophys Acta. 2009 Mar;1788(3):623-31. doi: 10.1016/j.bbamem.2008.12.014. Epub 2009 Jan 7.

Abstract

A key event in programmed cell death is the translocation of the apoptotic Bax protein from the cytosol towards mitochondria. The first helix localized at the N-terminus of Bax (Bax-alpha1) can act here as an addressing sequence, which directs activated Bax towards the mitochondrial surface. Solid state NMR (nuclear magnetic resonance), CD (circular dichroism) and ATR (attenuated total reflection) spectroscopy were used to elucidate this recognition process of a mitochondrial membrane system by Bax-alpha1. Two potential target membranes were studied, with the outer mitochondrial membrane (OM) mimicked by neutral phospholipids, while mitochondrial contact sites (CS) contained additional anionic cardiolipin. (1)H and (31)P magic angle spinning (MAS) NMR revealed Bax-alpha1 induced pronounced perturbations in the lipid headgroup region only in presence of cardiolipin. Bax-alpha1 could not insert into CS membranes but at elevated concentrations it inserted into the hydrophobic core of cardiolipin-free OM vesicles, thereby adopting beta-sheet-like features, as confirmed by ATR. CD studies revealed, that the cardiolipin mediated electrostatic locking of Bax-alpha1 at the CS membrane surface promotes conformational changes into an alpha-helical state; a process which seems to be necessary to induce further conformational transition events in activated Bax which finally causes irreversible membrane permeabilization during the mitochondrial apoptosis.

摘要

程序性细胞死亡中的一个关键事件是凋亡性Bax蛋白从细胞质向线粒体的转位。位于Bax N端的第一个螺旋(Bax-α1)在此可作为一个定位序列,将活化的Bax导向线粒体表面。利用固态核磁共振(NMR)、圆二色性(CD)和衰减全反射(ATR)光谱来阐明Bax-α1对线粒体膜系统的这种识别过程。研究了两种潜在的靶膜,用中性磷脂模拟线粒体外膜(OM),而线粒体接触位点(CS)含有额外的阴离子心磷脂。1H和31P魔角旋转(MAS)NMR显示,只有在心磷脂存在的情况下,Bax-α1才会在脂质头部区域引起明显的扰动。Bax-α1不能插入CS膜,但在高浓度下它会插入不含心磷脂的OM囊泡的疏水核心,从而呈现出β-折叠样特征,这一点已被ATR证实。CD研究表明,心磷脂介导的Bax-α1在CS膜表面的静电锁定促进了其构象转变为α-螺旋状态;这一过程似乎是诱导活化的Bax发生进一步构象转变事件所必需的,最终导致线粒体凋亡过程中不可逆的膜通透性改变。

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