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Smooth muscle myosin: regulation and properties

机译:平滑肌肌球蛋白:调节和特性

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摘要

The relationship of the biochemical states to the mechanical events in contraction of smooth muscle cross-bridges is reviewed. These studies use direct measurements of the kinetics of P-i and ADP release. The rate of release of P-i from thiophosphorylated cycling cross-bridges held isometric was biphasic with turnovers of 1.8 s(-1) and 0.3 s(-1), reflecting properties and forces directly acting on cross-bridges through mechanisms such as positive strain and inhibition by high-affinity MgADP binding. Fluorescent transients reporting release of an ADP analogue 3'-deac-edaADP were significantly faster in phasic than in tonic smooth muscles. Thiophosphorylation of myosin regulatory light chains (RLCs) increased and positive strain decreased the release rate around twofold. The rates of ADP release from rigor cross-bridges and the steady-state Pi release from cycling isometric cross-bridges are similar, indicating that the ADP-release step or an isomerization preceding it may limit the ATPase rate. Thus ADP release in phasic and tonic smooth muscles is a regulated step with strain- and dephosphorylation-dependence. High affinity; of cross-bridges for ADP and slow ADP release prolong the fraction of the duty cycle occupied by strongly, bound AM(.)ADP state(s) and contribute to the high economy of force that is characteristic of smooth muscle. RLC thiophosphorylation led to scructural changes in smooth muscle cross-bridges consistent with our findings that thiophosphorylation and strain modulate product release.
机译:综述了平滑肌横桥收缩过程中生物化学状态与机械事件的关系。这些研究直接测量了P-i和ADP释放的动力学。从等距的硫代磷酸化循环桥中释放Pi的速率是双相的,周转时间为1.8 s(-1)和0.3 s(-1),反映了特性和通过正应变和正电荷机制直接作用于桥上的力通过高亲和力的MgADP结合抑制。报告了ADP类似物3'-deac-edaADP释放的荧光瞬态在相态中比在平滑肌中快得多。肌球蛋白调节性轻链(RLC)的硫代磷酸化增加,阳性菌株降低释放速率约两倍。 ADP从严格的交叉桥释放的速率与稳态Pi从循环等距交叉桥释放的速率相似,这表明ADP释放步骤或之前的异构化可能会限制ATPase的速率。因此,ADP在有序和强直性平滑肌中的释放是依赖于应变和去磷酸化依赖性的调节步骤。高亲和力; ADP的跨桥和缓慢的ADP释放会延长强约束AM(。)ADP状态所占的工作周期,并有助于获得高效率的力,这是平滑肌的特征。 RLC硫代磷酸化导致平滑肌横桥的结构改变,这与我们的硫代磷酸化和菌株调节产物释放的发现一致。

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