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Cytoplasmic dynein binding run length and velocity are guided by long-range electrostatic interactions

机译:细胞质动力蛋白的结合游程长度和速度受远距离静电相互作用的指导

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摘要

Dyneins are important molecular motors involved in many essential biological processes, including cargo transport along microtubules, mitosis, and in cilia. Dynein motility involves the coupling of microtubule binding and unbinding to a change in the configuration of the linker domain induced by ATP hydrolysis, which occur some 25 nm apart. This leaves the accuracy of dynein stepping relatively inaccurate and susceptible to thermal noise. Using multi-scale modeling with a computational focusing technique, we demonstrate that the microtubule forms an electrostatic funnel that guides the dynein’s microtubule binding domain (MTBD) as it finally docks to the precise, keyed binding location on the microtubule. Furthermore, we demonstrate that electrostatic component of the MTBD’s binding free energy is linearly correlated with the velocity and run length of dynein, and we use this linearity to predict the effect of mutating each glutamic and aspartic acid located in MTBD domain to alanine. Lastly, we show that the binding of dynein to the microtubule is associated with conformational changes involving several helices, and we localize flexible hinge points within the stalk helices. Taken all together, we demonstrate that long range electrostatic interactions bring a level of precision to an otherwise noisy dynein stepping process.
机译:动力蛋白是重要的分子马达,参与​​许多必不可少的生物过程,包括沿微管,有丝分裂和纤毛的货物运输。动力蛋白的运动涉及微管结合和不结合与ATP水解诱导的接头结构域构型变化的耦合,ATP水解间隔约25nm。这使得达因步进的准确性相对不准确,并且容易受到热噪声的影响。通过使用具有计算聚焦技术的多尺度建模,我们证明了微管形成了一个静电漏斗,该漏斗会引导动力蛋白的微管结合域(MTBD)最终停靠在微管上的精确键控结合位置。此外,我们证明了MTBD结合自由能的静电成分与动力蛋白的速度和游程长度呈线性相关,并且我们利用此线性度来预测将MTBD域中的每个谷氨酸和天冬氨酸突变为丙氨酸的效果。最后,我们证明了动力蛋白与微管的结合与涉及几个螺旋的构象变化有关,并且我们在茎螺旋内定位了柔性铰链点。综上所述,我们证明了远距离静电相互作用为否则嘈杂的达因步进过程带来了一定的精确度。

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