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由白喉毒素在Vero细胞膜中形成的离子通道的结构-功能关系。

Structure-function relationship of the ion channel formed by diphtheria toxin in Vero cell membranes.

作者信息

Lanzrein M, Falnes P O, Sand O, Olsnes S

机构信息

Institute for Cancer Research, The Norwegian Radium Hospital, Montebello, 0310 Oslo, Norway.

出版信息

J Membr Biol. 1997 Mar 15;156(2):141-8. doi: 10.1007/s002329900196.

Abstract

Diphtheria toxin (DT) forms cation selective channels at low pH in cell membranes and planar bilayers. The channels formed by wild-type full length toxin (DT-AB), wild-type fragment B (DT-B) and mutants of DT-B were studied in the plasma membrane of Vero cells using the patch-clamp technique. The mutations concerned certain negatively charged amino acids within the channel-forming transmembrane domain (T-domain). These residues might interact electrostatically with cations flowing through the channel, and were therefore exchanged for uncharged amino acids or lysine. The increase in whole-cell conductance induced by toxin, Deltagm, was initially determined. DT-AB induced a approximately 10-fold lower Deltagm than DT-B. The mutations DT-B E327Q, DT-B D352N and DT-B E362K did not affect Deltagm, whereas DT-B D295K, DT-B D352K and DT-B D318K drastically reduced Deltagm. Single channel analysis of DT-B, DT-AB, DT-B D295K, DT-B D318K and DT-B E362K was then performed in outside-out patches. No differences were found for the single-channel conductances, but the mutants varied in their gating characteristics. DT-B D295K exhibited only a very transient channel activity. DT-AB as well as DT-B D318K displayed significantly lower open probability and mean dwell times than DT-B. Hence, the lower channel forming efficiency of DT-AB and DT-B D318K as compared to DT-B is reflected on the molecular level by their tendency to spend more time in the closed position and the fast flickering mode. Altogether, the present work shows that replacements of single amino acids distributed throughout a large part of the transmembrane domain (T-domain) strongly affect the overall channel activity expressed as Deltagm and the gating kinetics of single channels. This indicates clearly that the channel activity observed in DT-exposed Vero cells at low pH is inherent to DT itself and not due to DT-activation of an endogenous channel.

摘要

白喉毒素(DT)在细胞膜和平面双层膜的低pH值条件下形成阳离子选择性通道。利用膜片钳技术,在Vero细胞的质膜中研究了野生型全长毒素(DT-AB)、野生型片段B(DT-B)以及DT-B突变体所形成的通道。这些突变涉及通道形成跨膜结构域(T结构域)内的某些带负电荷的氨基酸。这些残基可能与流经通道的阳离子发生静电相互作用,因此被替换为不带电荷的氨基酸或赖氨酸。首先测定了毒素诱导的全细胞电导增加量ΔGm。DT-AB诱导的ΔGm比DT-B低约10倍。DT-B E327Q、DT-B D352N和DT-B E362K突变不影响ΔGm,而DT-B D295K、DT-B D352K和DT-B D318K则显著降低了ΔGm。然后在向外膜片上对DT-B、DT-AB、DT-B D295K、DT-B D318K和DT-B E362K进行单通道分析。单通道电导未发现差异,但突变体的门控特性有所不同。DT-B D29

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