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Thin filament cooperativity as a major determinant of shortening velocity in skeletal muscle fibers.

机译:细丝协同性是缩短骨骼肌纤维速度的主要决定因素。

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摘要

The mechanism underlying the calcium sensitivity of the velocity of shortening of skeletal muscle fibers was investigated using a multiple shortening protocol: within a single contraction, skinned rabbit psoas fibers were made to shorten repetitively under a light load by briefly stretching back to their initial length at regular intervals. At saturating [Ca2+], the initial fast shortening pattern was repeated reproducibly. At submaximal [Ca2+], the first shortening consisted of fast and slow phases, but only the slow phase was observed in later shortenings. When the fibers were held isometric after the first shortening, the velocity of the second shortening recovered with time. The recovery paralleled tension redevelopment, implying a close relationship between the velocity and the number of the preexisting force-producing cross-bridges. However, this parallelism was lost as [Ca2+] was increased. Thus, the velocity was modified in a manner consistent with the cooperative thin filament activation by strong binding cross-bridges and its modulation by calcium. The present results therefore provide evidence that the thin filament cooperativity is primarily responsible for the calcium sensitivity of velocity. The effect of inorganic phosphate to accelerate the slow phase of shortening is also explained in terms of the cooperative activation.
机译:使用多种缩短方案研究了骨骼肌纤维缩短速度对钙敏感性的潜在机制:在单次收缩中,通过轻拉伸将其恢复至初始长度,在轻负荷下使去皮的兔腰大肌纤维重复缩短。定期间隔。在[Ca2 +]饱和时,可重复地重复最初的快速缩短模式。在[Ca2 +]小于最大值时,第一个起酥油由快和慢相组成,但在随后的起酥油中仅观察到了慢相。第一次缩短后,当纤维保持等距时,第二次缩短的速度随时间恢复。恢复与张力再发展平行,这意味着速度和预先存在的产生力的跨桥的数量之间存在密切的关系。但是,随着[Ca2 +]的增加,这种平行性消失了。因此,以与通过强结合横桥的协同细丝活化和钙的调节相一致的方式来改变速度。因此,目前的结果提供了证据,证明细丝的协同作用是速度钙敏感性的主要原因。还通过协同活化解释了无机磷酸盐促进起酥油的缓慢相的作用。

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