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与平滑肌Ca2+敏感性相关的rhoA易位。

Translocation of rhoA associated with Ca2+ sensitization of smooth muscle.

作者信息

Gong M C, Fujihara H, Somlyo A V, Somlyo A P

机构信息

Department of Molecular Physiology and Biological Physics, University of Virginia Health Sciences Center, Charlottesville, Virginia 22906-0011, USA.

出版信息

J Biol Chem. 1997 Apr 18;272(16):10704-9. doi: 10.1074/jbc.272.16.10704.

Abstract

We determined the relationship between the localization of rhoA and Ca2+ sensitization of force in smooth muscle. In alpha-toxin-permeabilized rabbit portal vein at pCa 6.5, the particulate hydrophobic fraction of rhoA (10 +/- 1.6% of the total) was significantly increased by phenylephrine to 18 +/- 5.5% at 5 min, by AlF4- to 26 +/- 8.4% at 20 min, and dose-dependently up to 62 +/- 9.5% by guanosine 5'-O-(3-thiotriphosphate) (GTPgammaS; 0.3-50 microM). Translocation of rhoA was selective (Rac1 and Cdc42 were not translocated) and was quantitatively correlated (up to approximately 50%; r = 0.91, p < 0.05) with Ca2+ sensitization; high GTPgammaS concentrations (>/=10 microM) further increased translocation without increasing force. The initial recruitment of rhoA to the membrane paralleled the time course of contraction, but sensitization could be reversed without a decrease in particulate rhoA. High [Ca2+] (pCa 4.5) also increased particulate rhoA to 31 +/- 5.8%. Membrane-associated rhoA in unstimulated portal vein was a good substrate for in vitro ADP-ribosylation, whereas the large amount translocated by GTPgammaS was not. We conclude that 1) translocation of rhoA plays a causal role in Ca2+ sensitization, and 2) membrane-bound rhoA can exist in two or more states.

摘要

我们确定了RhoA的定位与平滑肌中力的Ca2+敏化之间的关系。在pCa 6.5的α-毒素通透的兔门静脉中,苯肾上腺素可使RhoA的颗粒疏水部分(占总量的10±1.6%)在5分钟时显著增加至18±5.5%,AlF4-可使其在20分钟时增加至26±8.4%,而鸟苷5'-O-(3-硫代三磷酸)(GTPγS;0.3 - 50μM)可使其剂量依赖性地增加至62±9.5%。RhoA的易位具有选择性(Rac1和Cdc42未发生易位),并且与Ca2+敏化在数量上相关(高达约50%;r = 0.91,p < 0.05);高浓度的GTPγS(≥10μM)进一步增加易位但不增加力。RhoA最初募集到膜上的过程与收缩的时间进程平行,但敏化可以逆转而颗粒RhoA不减少。高[Ca2+](pCa 4.5)也可使颗粒RhoA增加至31±5.8%。未刺激的门静脉中与膜相关的RhoA是体外ADP-核糖基化的良好底物,而由GTPγS易位的大量RhoA则不是。我们得出结论:1)RhoA的易位在Ca2+敏化中起因果作用;2)膜结合的RhoA可以以两种或更多种状态存在。

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