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钙调蛋白和钙结合蛋白磷酸化在平滑肌收缩调节中的作用

Caldesmon and calponin phosphorylation in regulation of smooth muscle contraction.

作者信息

Gerthoffer W T, Pohl J

机构信息

Department of Pharmacology, University of Nevada School of Medicine, Reno 89557-0046, USA.

出版信息

Can J Physiol Pharmacol. 1994 Nov;72(11):1410-4. doi: 10.1139/y94-203.

Abstract

Recent studies of the smooth muscle contractile system indicate that Ca(2+)-dependent phosphorylation of the 20-kDa myosin light chains, modulation of phosphoprotein phosphatases, and phosphorylation of thin-filament proteins are all potential features of contractile system regulation. The thin-filament proteins caldesmon and calponin are known to inhibit actomyosin ATPase in vitro and actin sliding velocity in the in vitro motility assay. Inhibition of actomyosin ATPase is relieved by phosphorylation of caldesmon or calponin. The notion that caldesmon and calponin phosphorylation-dephosphorylation is important in the living smooth muscle cell was tested using canine tracheal smooth muscle strips labeled with 32P. We found that both caldesmon and calponin phosphorylation increased in response to stimulation with carbachol. Carbachol induced a biphasic increase in [Ca2+]i in canine tracheal smooth muscle, an early transient increase in myosin phosphorylation, which decayed to 0.4 mol Pi/mol light chain, and a rapid transient increase in tissue shortening velocity. Relative changes in caldesmon phosphorylation correlate best with force development and the [Ca2+]i transient, both of which follow a similar time course. Calponin phosphorylation appears to be a rapid transient event more similar to the transient increase in unloaded shortening velocity. Our results are consistent with a potential role for both caldesmon and calponin phosphorylation in regulating smooth muscle contraction.

摘要

近期对平滑肌收缩系统的研究表明,20 kDa肌球蛋白轻链的钙依赖性磷酸化、磷蛋白磷酸酶的调节以及细肌丝蛋白的磷酸化都是收缩系统调节的潜在特征。已知细肌丝蛋白钙调蛋白和钙泊宁在体外可抑制肌动球蛋白ATP酶,并在体外运动分析中抑制肌动蛋白滑动速度。钙调蛋白或钙泊宁的磷酸化可解除对肌动球蛋白ATP酶的抑制。我们使用用32P标记的犬气管平滑肌条来测试钙调蛋白和钙泊宁磷酸化-去磷酸化在活的平滑肌细胞中是否重要这一观点。我们发现,用卡巴胆碱刺激后,钙调蛋白和钙泊宁的磷酸化均增加。卡巴胆碱可诱导犬气管平滑肌中[Ca2+]i出现双相增加,肌球蛋白磷酸化出现早期短暂增加,随后衰减至0.4 mol Pi/mol轻链,同时组织缩短速度出现快速短暂增加。钙调蛋白磷酸化的相对变化与力的产生以及[Ca2+]i瞬变最为相关,二者均遵循相似的时间进程。钙泊宁磷酸化似乎是一个快速短暂事件,更类似于无负荷缩短速度的短暂增加。我们的结果与钙调蛋白和钙泊宁磷酸化在调节平滑肌收缩中具有潜在作用这一观点一致。

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