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横桥循环的调节:MgADP、LC17 同工型和端激酶的作用。

Regulation of the cross-bridge cycle: the effects of MgADP, LC17 isoforms and telokin.

作者信息

Somlyo A V, Matthew J D, Wu X, Khromov A S, Somlyo A P

机构信息

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

出版信息

Acta Physiol Scand. 1998 Dec;164(4):381-8. doi: 10.1111/j.1365-201x.1998.tb10695.x.

Abstract

This review summarizes the role of MgADP in force maintenance by dephosphorylated cross-bridges in smooth muscle and a potential physiological role for telokin. In tonic, compared with phasic, smooth muscles the affinity of cross-bridges in approximately 5 times higher for MgADP and the apparent second-order rate constant for MgATP is approximately 3 times lower. This gives rise to a large population of dephosphorylated cross-bridges in tonic smooth muscle. Such cross-bridges are thought to be major determinants of the different relaxation kinetics of the two types of smooth muscle and contribute to force maintenance at low levels of MLC20 phosphorylation, termed 'catch-like state' (Somlyo & Somlyo 1967) or 'latch' (Dillon et al. 1981). The molecular basis of the different affinities for MgADP and MgATP between tonic and phasic smooth muscle myosin was explored by exchange of essential myosin light chain (LC17) isoforms. In phasic bladder smooth muscle the exchange of LC17b for LC17a caused a significant decrease in the unloaded shortening velocity of non-phosphorylated, slowly cycling cross-bridges, suggesting that the LC17 isoforms contribute to the nucleotide affinity of latch bridges. The role of telokin in Ca(2+)-desensitization in phasic smooth muscle is reviewed. Telokin, the independently expressed C-terminus of myosin light chain kinase, is extensively phosphorylated during forskolin- and 8-br-cGMP-induced relaxation in situ. Telokin accelerated dephosphorylation of the regulatory myosin light chain and relaxed rabbit ileum smooth muscle. The results suggest that telokin contributes to cAMP and/or cGMP kinase-mediated Ca(2+)-desensitization of phasic smooth muscles.

摘要

本综述总结了MgADP在平滑肌中去磷酸化横桥维持张力方面的作用以及telokin的潜在生理作用。在张力性平滑肌中,与相性平滑肌相比,横桥对MgADP的亲和力大约高5倍,而对MgATP的表观二级速率常数大约低3倍。这导致张力性平滑肌中存在大量去磷酸化横桥。这类横桥被认为是两种平滑肌不同舒张动力学的主要决定因素,并有助于在低水平肌球蛋白轻链20(MLC20)磷酸化时维持张力,即所谓的“类捕获状态”(索姆利奥和索姆利奥,1967年)或“闩锁状态”(狄龙等人,1981年)。通过交换必需肌球蛋白轻链(LC17)同工型,探讨了张力性和平相性平滑肌肌球蛋白对MgADP和MgATP不同亲和力的分子基础。在相性膀胱平滑肌中,将LC17b换成LC17a会导致非磷酸化、缓慢循环横桥的无负荷缩短速度显著降低,这表明LC17同工型有助于闩锁横桥的核苷酸亲和力。本文综述了telokin在相性平滑肌钙脱敏中的作用。Telokin是肌球蛋白轻链激酶独立表达的C末端,在福斯可林和8-溴-cGMP诱导的原位舒张过程中会发生广泛磷酸化。Telokin加速了调节性肌球蛋白轻链的去磷酸化,并使兔回肠平滑肌舒张。结果表明,telokin有助于cAMP和/或cGMP激酶介导的相性平滑肌钙脱敏。

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