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脂双层中短杆菌肽通道形成的动力学:跨膜单体缔合

Kinetics of gramicidin channel formation in lipid bilayers: transmembrane monomer association.

作者信息

O'Connell A M, Koeppe R E, Andersen O S

机构信息

Department of Physiology and Biophysics, Cornell University Medical College, New York, NY 10021.

出版信息

Science. 1990 Nov 30;250(4985):1256-9. doi: 10.1126/science.1700867.

Abstract

Conducting gramicidin channels form predominantly by the transmembrane association of monomers, one from each side of a lipid bilayer. In single-channel experiments in planar bilayers the two gramicidin analogs, [Val1]gramicidin A (gA) and [4,4,4-F3-Val1]gramicidin A (F3gA), form dimeric channels that are structurally equivalent and have characteristically different conductances. When these gramicidins were added asymmetrically, one to each side of a preformed bilayer, the predominant channel type was the hybrid channel, formed between two chemically dissimilar monomers. These channels formed by the association of monomers residing in each half of the membrane. These results also indicate that the hydrophobic gramicidins are surprisingly membrane impermeant, a conclusion that was confirmed in experiments in which gA was added asymmetrically and symmetrically to preformed bilayers.

摘要

短杆菌肽通道主要由单体的跨膜缔合形成,每个单体来自脂质双层的一侧。在平面双层的单通道实验中,两种短杆菌肽类似物,[Val1]短杆菌肽A(gA)和[4,4,4-F3-Val1]短杆菌肽A(F3gA),形成结构等效但电导率特征不同的二聚体通道。当这些短杆菌肽不对称地添加到预先形成的双层的每一侧时,主要的通道类型是杂合通道,由两个化学性质不同的单体之间形成。这些通道由位于膜各半侧的单体缔合形成。这些结果还表明,疏水性短杆菌肽令人惊讶地不能透过膜,这一结论在将gA不对称和对称地添加到预先形成的双层的实验中得到了证实。

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