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猪心脏亚片段-1的生化动力学

Biochemical kinetics of porcine cardiac subfragment-1.

作者信息

Stein L A, White M P

出版信息

Circ Res. 1987 Jan;60(1):39-49. doi: 10.1161/01.res.60.1.39.

DOI:10.1161/01.res.60.1.39
PMID:2952363
Abstract

The actin binding and ATPase kinetics of cardiac myosin subfragment-1 were compared with prior studies on skeletal myosin subfragments. Previous kinetic studies on rabbit skeletal subfragment-1 (S-1) have revealed two important features of the actomyosin ATPase activity. First, hydrolysis of ATP by myosin subfragment-1 proceeds both when S-1 is bound to actin and when it is dissociated from actin. Second, the actin concentration required to reach half the maximum ATPase activity, Ka(ATPase), is considerably lower than the actin concentration required to bind half the subfragment-1 during steady state hydrolysis of ATP, Ka(binding). These kinetic facts require that skeletal myosin hydrolyze ATP without dissociating from actin; therefore, a "nondissociating" pathway for ATP hydrolysis exists. The studies reported here show that porcine cardiac S-1 is very similar to rabbit skeletal S-1. Under identical conditions to prior work on skeletal S-1, the Ka(ATPase) of porcine cardiac S-1 is approximately equal to that reported for skeletal S-1. This is also true for Ka(binding). Comparison of Ka(ATPase) and Ka(binding) shows that for cardiac proteins Ka(ATPase) is fourfold to sixfold stronger than Ka(binding), i.e., half maximal ATPase activity is achieved at about one fifth the actin necessary to reach 50% binding. The extrapolated maximum ATPase activity at saturating actin concentration for cardiac S-1 is consistently slower than skeletal S-1 by about a factor of 2.5. Furthermore, studies of the actoS-1 ATPase activity at high actin concentrations as well as with crosslinked actoS-1 show no significant inhibition, implying the requirement of a "nondissociating" pathway for ATP hydrolysis by cardiac myosin subfragment-1.

摘要

将心肌肌球蛋白亚片段-1的肌动蛋白结合和ATP酶动力学与之前对骨骼肌肌球蛋白亚片段的研究进行了比较。先前对兔骨骼肌亚片段-1(S-1)的动力学研究揭示了肌动球蛋白ATP酶活性的两个重要特征。首先,当S-1与肌动蛋白结合以及从肌动蛋白解离时,肌球蛋白亚片段-1都会进行ATP水解。其次,达到最大ATP酶活性一半时所需的肌动蛋白浓度Ka(ATPase),远低于在ATP稳态水解过程中结合一半亚片段-1所需的肌动蛋白浓度Ka(结合)。这些动力学事实表明,骨骼肌肌球蛋白在不解离肌动蛋白的情况下水解ATP;因此,存在ATP水解的“不解离”途径。本文报道的研究表明,猪心肌S-1与兔骨骼肌S-1非常相似。在与先前对骨骼肌S-1研究相同的条件下,猪心肌S-1的Ka(ATPase)大约等于报道的骨骼肌S-1的Ka(ATPase)。Ka(结合)也是如此。Ka(ATPase)和Ka(结合)的比较表明,对于心脏蛋白,Ka(ATPase)比Ka(结合)强4至6倍,即达到最大ATP酶活性一半时所需的肌动蛋白浓度约为达到50%结合所需肌动蛋白浓度的五分之一。在肌动蛋白浓度饱和时,心肌S-1的外推最大ATP酶活性始终比骨骼肌S-1慢约2.5倍。此外,在高肌动蛋白浓度下以及对交联的肌动蛋白-S-1进行的肌动蛋白-S-1 ATP酶活性研究均未显示出明显抑制,这意味着心肌肌球蛋白亚片段-1进行ATP水解需要“不解离”途径。

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