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对由病毒融合蛋白介导的单细胞融合事件的膜片钳研究。

Patch clamp studies of single cell-fusion events mediated by a viral fusion protein.

作者信息

Spruce A E, Iwata A, White J M, Almers W

机构信息

Department of Physiology and Biophysics, University of Washington, Seattle 98195.

出版信息

Nature. 1989 Nov 30;342(6249):555-8. doi: 10.1038/342555a0.

Abstract

To enter cells, viruses must fuse their envelope with a host cell membrane. Fusion is mediated by specific, membrane-spanning fusion proteins, of which the influenza virus haemagglutinins (HA) are the best characterized. Several HAs have been sequenced, and the crystal structure of the major part of one HA is known. The conditions for fusion and some of the rearrangements in the HA that accompany fusion are well understood, but it remains unclear how HA causes bilayers to fuse. We have observed, in real time, unitary cell-fusion events caused by HA. Fibroblasts expressing HA were induced to fuse with red blood cells by a rapid drop in pH. Fusion was monitored by fluorescence microscopy, and by measuring the membrane conductance and capacitance of the fibroblast. The earliest event observed was the sudden opening of an aqueous pore connecting the cytoplasms of the fusing cells. Initially, the pore conductance often fluctuated between zero and approximately 600 pS, as if the pore were opening and closing repeatedly. Later, it increased over tens of seconds, as if the pore dilated. We suggest that, as in exocytosis, HA-mediated membrane fusion begins with the formation of a narrow pore. Based on the conductance, we estimate the initial diameter of the pore to be no more than twice that of a gap junction channel.

摘要

病毒要进入细胞,就必须使其包膜与宿主细胞膜融合。融合由特定的跨膜融合蛋白介导,其中流感病毒血凝素(HA)的特征最为明确。几种HA已被测序,且一种HA主要部分的晶体结构也已为人所知。融合的条件以及HA在融合过程中发生的一些重排已被充分了解,但HA如何导致双层膜融合仍不清楚。我们实时观察到了由HA引起的单细胞融合事件。表达HA的成纤维细胞通过pH值的快速下降被诱导与红细胞融合。通过荧光显微镜以及测量成纤维细胞的膜电导和电容来监测融合过程。观察到的最早事件是连接融合细胞细胞质的水相孔道突然打开。最初,孔道电导常常在零和大约600皮西门子之间波动,就好像孔道在反复开闭。后来,它在数十秒内增加,就好像孔道在扩张。我们认为,与胞吐作用一样,HA介导的膜融合始于窄孔道的形成。根据电导,我们估计孔道的初始直径不超过间隙连接通道直径的两倍。

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