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首页> 外文期刊>Archives of Biochemistry and Biophysics >Nucleotide-free kinesin motor domains reversibly convert to an inactive conformation with characteristics of a molten globule
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Nucleotide-free kinesin motor domains reversibly convert to an inactive conformation with characteristics of a molten globule

机译:无核苷酸的驱动蛋白运动域可逆地转化为具有熔融小球特征的非活性构象

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摘要

Nucleotide-free kinesin motor domains from several kinesin families convert reversibly to a refractory conformation that cannot rapidly rebind ADP. In the absence of glycerol, the refractory conformation of Drosophila kinesin motor domains is favored by 50-fold with conversion of the active to the refractory species at similar to 0.052 s(-1) and reactivating in the presence of ADP at similar to 0.001 s(-1). This reactivation by ADP is due to conformational selection rather than induced fit because ADP is not bound to the refractory species at concentrations of ADP that are sufficient to saturate the rate of reactivation. Glycerol stabilizes the active conformation by reducing the rate of inactivation, while having little effect on the reactivation rate. Circular dichroism indicates a large conformational change occurs on formation of the refractory species. The refractory conformation binds ANS (8-anilino-1-napthalenesulfonic acid) with a large increase in fluorescence, indicating that it has molten globule character. High ANS binding is also observed with the refractory forms of Eg5 (a kinesin-5) and Ncd (a kinesin-14), indicating that a refractory conformation with molten globule characteristics may be a common feature of nucleotide-free kinesin motor domains. (C) 2016 Elsevier Inc. All rights reserved.
机译:来自几个驱动蛋白家族的无核苷酸驱动蛋白运动域可逆地转化为不能快速结合ADP的难治性构象。在不存在甘油的情况下,果蝇驱动蛋白运动结构域的难治性构象受到50倍青睐,其中活性物质转化为难治性物种的转化率接近0.052 s(-1),并在ADP存在下于0.001 s活化(-1)。 ADP的这种再活化是由于构象选择而不是诱导的拟合,因为在足以饱和再活化速率的ADP浓度下,ADP不会结合到耐火物质上。甘油通过降低失活速率来稳定活性构象,而对再活化速率几乎没有影响。圆二色性表明在形成耐火物质时发生了较大的构象变化。难熔构象结合ANS(8-苯胺基-1-萘磺酸),并具有较大的荧光增强,表明它具有熔融的球状特征。 Eg5(驱动蛋白5)和Ncd(驱动蛋白14)的难治性形式也观察到了高度的ANS结合,表明具有熔融小球特征的难治性构象可能是无核苷酸的驱动蛋白运动域的共同特征。 (C)2016 Elsevier Inc.保留所有权利。

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