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HIV-1包膜蛋白在融合孔形成后立即完成折叠形成六螺旋束。

HIV-1 envelope proteins complete their folding into six-helix bundles immediately after fusion pore formation.

作者信息

Markosyan Ruben M, Cohen Fredric S, Melikyan Grigory B

机构信息

Department of Molecular Biophysics and Physiology, Rush Medical College, Chicago, Illinois 60612, USA.

出版信息

Mol Biol Cell. 2003 Mar;14(3):926-38. doi: 10.1091/mbc.e02-09-0573.

Abstract

Fusion proteins of many viruses, including HIV-1 envelope protein (Env), fold into six-helix bundle structures. Fusion between individual Env-expressing cells and target cells was studied by fluorescence microscopy, and a temperature jump technique, to determine whether folding of Env into a bundle is complete by the time fusion pores have formed. Lowering temperature to 4 degrees C immediately after a pore opened halted pore growth, which quickly resumed when temperature was raised again. HIV gp41-derived peptides that inhibit bundle formation (C34 or N36) caused the cold-arrested pore to quickly and irreversibly close, demonstrating that bundle formation is not complete by the time a pore has formed. In contrast, lowering the temperature to an intermediate value also halted pore growth, but the pore was not closed by the bundle-inhibiting peptides, and it enlarged when temperature was again elevated. This latter result shows that bundle formation is definitely required for the fusion process, but surprisingly, some (if not all) bundle formation occurs after a pore has formed. It is concluded that an essential function of the bundle is to stabilize the pore against collapse and ensure its growth.

摘要

包括HIV-1包膜蛋白(Env)在内的许多病毒的融合蛋白会折叠成六螺旋束结构。通过荧光显微镜和温度跳跃技术研究了单个表达Env的细胞与靶细胞之间的融合,以确定在融合孔形成时Env折叠成束的过程是否已经完成。在孔打开后立即将温度降至4摄氏度会阻止孔的生长,当温度再次升高时,孔的生长会迅速恢复。抑制束形成的HIV gp41衍生肽(C34或N36)会导致冷阻滞的孔迅速且不可逆地关闭,这表明在孔形成时束的形成尚未完成。相比之下,将温度降至中间值也会阻止孔的生长,但束抑制肽不会使孔关闭,当温度再次升高时孔会扩大。后一个结果表明融合过程肯定需要束的形成,但令人惊讶的是,一些(如果不是全部)束的形成发生在孔形成之后。得出的结论是,束的一个基本功能是稳定孔以防其塌陷并确保其生长。

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