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通过DNA序列和微管结合分析揭示的驱动蛋白重链的三结构域结构。

A three-domain structure of kinesin heavy chain revealed by DNA sequence and microtubule binding analyses.

作者信息

Yang J T, Laymon R A, Goldstein L S

机构信息

Department of Cellular and Developmental Biology, Harvard University, Cambridge, Massachusetts 02138.

出版信息

Cell. 1989 Mar 10;56(5):879-89. doi: 10.1016/0092-8674(89)90692-2.

Abstract

The structure and function of kinesin heavy chain from D. melanogaster have been studied using DNA sequence analysis and analysis of the properties of truncated kinesin heavy chain synthesized in vitro. Analysis of the sequence suggests the existence of a 50 kd globular amino-terminal domain that contains an ATP binding consensus sequence, followed by another 50-60 kd domain that has sequence characteristics consistent with the ability to fold into an alpha helical coiled coil. The properties of amino- and carboxy-terminally truncated kinesin heavy chains synthesized in vitro reveal that a 60 kd amino-terminal fragment has the nucleotide-dependent microtubule binding activities of the intact kinesin heavy chain, and hence is likely to be a "motor" domain. Finally, the sequence data indicate the presence of a small carboxy-terminal domain. Because it is located at the end of the molecule away from the putative "motor" domain, we propose that this domain is responsible for interactions with other proteins, vesicles, or organelles. These data suggest that kinesin has an organization very similar to that of myosin even though there are no obvious sequence similarities between the two molecules.

摘要

利用DNA序列分析以及对体外合成的截短型驱动蛋白重链性质的分析,对黑腹果蝇驱动蛋白重链的结构和功能进行了研究。序列分析表明,存在一个50kd的球状氨基末端结构域,其中包含一个ATP结合共有序列,随后是另一个50 - 60kd的结构域,其序列特征与折叠成α螺旋卷曲螺旋的能力一致。体外合成的氨基末端和羧基末端截短的驱动蛋白重链的性质表明,一个60kd的氨基末端片段具有完整驱动蛋白重链的核苷酸依赖性微管结合活性,因此可能是一个“运动”结构域。最后,序列数据表明存在一个小的羧基末端结构域。由于它位于远离假定“运动”结构域的分子末端,我们认为该结构域负责与其他蛋白质、囊泡或细胞器的相互作用。这些数据表明,驱动蛋白的结构组织与肌球蛋白非常相似,尽管这两种分子之间没有明显的序列相似性。

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