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人类CksHs2的原子结构:其六聚体组装在细胞周期调控中的作用。

Human CksHs2 atomic structure: a role for its hexameric assembly in cell cycle control.

作者信息

Parge H E, Arvai A S, Murtari D J, Reed S I, Tainer J A

机构信息

The Department of Molecular Biology, Scripps Research Institute, La Jolla, CA 92037.

出版信息

Science. 1993 Oct 15;262(5132):387-95. doi: 10.1126/science.8211159.

Abstract

The cell cycle regulatory protein CksHs2 binds to the catalytic subunit of the cyclin-dependent kinases (Cdk's) and is essential for their biological function. The crystal structure of the protein was determined at 2.1 A resolution. The CksHs2 structure is an unexpected hexamer formed by the symmetric assembly of three interlocked dimers into an unusual 12-stranded beta barrel fold that may represent a prototype for this class of protein structures. Sequence-conserved regions form the unusual beta strand exchange between the subunits of the dimer, and the metal and anion binding sites associated with the hexamer assembly. The two other sequence-conserved regions line a 12 A diameter tunnel through the beta barrel and form the six exposed, charged helix pairs. Six kinase subunits can be modeled to bind the assembled hexamer without collision, and therefore this CksHs2 hexamer may participate in cell cycle control by acting as the hub for Cdk multimerization in vivo.

摘要

细胞周期调节蛋白CksHs2与细胞周期蛋白依赖性激酶(Cdk)的催化亚基结合,对其生物学功能至关重要。该蛋白的晶体结构以2.1埃的分辨率测定。CksHs2结构出人意料地是一个六聚体,由三个互锁的二聚体对称组装成一个不寻常的12股β桶状折叠,这可能代表了这类蛋白质结构的一个原型。序列保守区域形成二聚体亚基之间不寻常的β链交换,以及与六聚体组装相关的金属和阴离子结合位点。另外两个序列保守区域沿着穿过β桶的直径为12埃的通道排列,并形成六个暴露的带电荷螺旋对。可以模拟六个激酶亚基与组装好的六聚体结合而不发生碰撞,因此这种CksHs2六聚体可能通过在体内作为Cdk多聚化的中心来参与细胞周期控制。

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