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Does the intercept of the heat-stress relation provide an accurate estimate of cardiac activation heat?

机译:热应激关系的截距是否提供了对心脏活化热的准确估计?

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Activation heat arises from two sources during the contraction of striated muscle. It reflects the metabolic expenditure associated with Ca2+ pumping by the sarcoplasmic reticular Ca2+-ATPase and Ca2+ translocation by the Na+/Ca2+ exchanger coupled to the Na+,K+-ATPase. In cardiac preparations, investigators are constrained in estimating its magnitude by reducing muscle length to the point where macroscopic twitch force vanishes. But this experimental protocol has been criticised since, at zero force, the observed heat may be contaminated by residual crossbridge cycling activity. To eliminate this concern, the putative thermal contribution from crossbridge cycling activity must be abolished, at least at minimal muscle length. We achieved this using blebbistatin, a selective inhibitor of myosin II ATPase. Using a microcalorimeter, we measured the force production and heat output, as functions of muscle length, of isolated rat trabeculae from both ventricles contracting isometrically at 5 Hz and at 37 degrees C. In the presence of blebbistatin (15 mu mol l(-1)), active force was zero but heat output remained constant, at all muscle lengths. Activation heat measured in the presence of blebbistatin was not different from that estimated from the intercept of the heat-stress relation in its absence. We thus reached two conclusions. First, activation heat is independent of muscle length. Second, residual crossbridge heat is negligible at zero active force; hence, the intercept of the cardiac heat-force relation provides an estimate of activation heat uncontaminated by crossbridge cycling. Both results resolve long-standing disputes in the literature.
机译:在条纹肌肉收缩期间,激活热量由两个来源产生。它反映了与肌肉网状网状Ca2 + -AtPase和Ca2 +通过偶联至Na +,K + -AtPase的Na + / Ca2 +交换剂泵送相关的代谢支出。在心脏准备中,调查人员通过将肌肉长度降低到宏观抽搐力消失的点来限制估计其幅度。但是,这种实验方案已经受到批评,因为在零力下,观察到的热量可能被残留的横梁循环活性污染。为了消除这种问题,必须至少在最小的肌肉长度下消除来自跨桥循环活性的推定的热贡献。我们使用Blebbistatin,一种肌球蛋白II ATPase的选择性抑制剂实现了这一点。使用微量微量计,我们测量了来自在5Hz的空常性和37摄氏度的肌肉长度的肌肉长度的功能,作为肌肉长度的肌肉长度的函数。在Blebbistatin(15μmoll(-1)存在下)),有源力为零,但热输出保持恒定,在所有肌肉长度。在Blebbistatin的存在下测量的活化热与其缺失的热应激关系截距的估计没有不同。因此,我们得出了两次结论。首先,激活热与肌肉长度无关。其次,剩余的横梁热量在零主动力可忽略不计;因此,心脏热力关系的截距提供了由跨界循环无污染的活化热的估计。这两个结果都解决了文献中的长期争端。

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