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The Kinetic Mechanism of Mouse Myosin VIIA

机译:小鼠肌球蛋白志中的动力学机制

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Myosin VIIa is crucial in hearing and visual processes. We examined the kinetic and association properties of the baculovirus expressed, truncated mouse myosin VIIa construct containing the head, all 5IQ motifs and the putative coiled coil domain (myosin VIIa-5IQ). The construct appears to be monomeric as determined by analytical ultracentrifugation experiments, and only single headed molecules were detected by negative stain electron microscopy. The relatively high basal steady-state rate of 0.18 s?1 is activated by actin only by ~3.5-fold resulting in a Vmax of 0.7 s?1 and a KATPase of 11.5 μm. There is no single rate-limiting step of the ATP hydrolysis cycle. The ATP hydrolysis step (M·T ? M·D·P) is slow (12 s?1) and the equilibrium constant (KH) of 1 suggests significant reversal of hydrolysis. In the presence of actin ADP dissociates with a rate constant of 1.2 s?1. Phosphate dissociation is relatively fast (>12 s?1), but the maximal rate could not be experimentally obtained at actin concentrations ≤ 50 μm because of the weak binding of the myosin VIIa-ADP-Pi complex to actin. At higher actin concentrations the rate of attached hydrolysis (0.4 s?1) becomes significant and partially rate-limiting. Our findings suggest that the myosin VIIa is a “slow”, monomeric molecular motor with a duty ratio of 0.6.
机译:肌球蛋白VIIA在听证和视觉过程中至关重要。我们检查了杆状病毒表达的动力学和结合性质,截断小鼠肌苷VIIA构建体,含有头部,所有5IQ基序和推定的卷绕卷域(Myosin VIIA-5IQ)。构建体似乎是单体,如通过分析超速离心实验确定,并且仅通过负染色电子显微镜检测单个头部分子。通过肌动蛋白激活的相对较高的基底稳态速率为0.18秒的致动蛋白〜3.5倍,得到0.7℃的Vmax和11.5μm的katpase。 ATP水解循环没有单一速率限制步骤。 ATP水解步骤(M·T→M·D·D·D·P)是慢(12秒1),1的平衡常数(kH)表明水解的显着逆转。在肌动蛋白ADP存在下解离速率常数为1.2 s?1。磷酸盐解离相对较快(> 12s≤1),但由于肌球蛋白viia-aadp-pi复合物与肌动蛋白的弱结合,因此不能在actin浓度≤50μm处实验获得最大速率。在较高的肌动蛋白浓度下,附着水解的速率(0.4秒1)变得显着且部分速率限制。我们的研究结果表明,肌球蛋白viia是一个“慢”,单体分子电机,占空比为0.6。

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