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人类纺锤体蛋白1的结构。用于细胞周期调控的串联类 Tudor 结构域。

Structure of human spindlin1. Tandem tudor-like domains for cell cycle regulation.

作者信息

Zhao Qiang, Qin Lipeng, Jiang Fuguo, Wu Beili, Yue Wen, Xu Feng, Rong Zhili, Yuan Hongfeng, Xie Xiaoyan, Gao Yanhong, Bai Cixian, Bartlam Mark, Pei Xuetao, Rao Zihe

机构信息

Tsinghua-Institute of Biophysics Joint Research Group for Structural Biology, Tsinghua University, Beijing 100084, China.

出版信息

J Biol Chem. 2007 Jan 5;282(1):647-56. doi: 10.1074/jbc.M604029200. Epub 2006 Nov 1.

Abstract

Spindlin1, a meiotic spindle-binding protein that is highly expressed in ovarian cancer cells, was first identified as a gene involved in gametogenesis. It appeared to be a target for cell cycle-dependent phosphorylation and was demonstrated to disturb the cell cycle. Here we report the crystal structure of human spindlin1 to 2.2A of resolution, representing the first three-dimensional structure from the spin/ssty (Y-linked spermiogenesis-specific transcript) gene family. The refined structure, containing three repeats of five/four anti-parallel beta-strands, exhibits a novel arrangement of tandem Tudor-like domains. Two phosphate ions, chelated by Thr-95 and other residues, appear to stabilize the long loop between domains I and II, which might mediate the cell cycle regulation activity of spindlin1. Flow cytometry experiments indicate that cells expressing spindlin1 display a different cell cycle distribution in mitosis, whereas those expressing a T95A mutant, which had a great decrease in phosphorous content, have little effect on the cell cycle. We further identified associations of spindlin1 with nucleic acid to provide a biochemical basis for its cell cycle regulation and other functions.

摘要

Spindlin1是一种在卵巢癌细胞中高表达的减数分裂纺锤体结合蛋白,最初被鉴定为参与配子发生的基因。它似乎是细胞周期依赖性磷酸化的靶点,并被证明会干扰细胞周期。在此,我们报道了人Spindlin1的晶体结构,分辨率为2.2埃,这是spin/ssty(Y连锁精子发生特异性转录本)基因家族的首个三维结构。优化后的结构包含三个由五个/四个反平行β链组成的重复序列,呈现出串联类 Tudor 结构域的新颖排列。由苏氨酸-95和其他残基螯合的两个磷酸离子似乎稳定了结构域I和II之间的长环,这可能介导了Spindlin1的细胞周期调节活性。流式细胞术实验表明,表达Spindlin1的细胞在有丝分裂中表现出不同的细胞周期分布,而表达磷含量较低的T95A突变体的细胞对细胞周期几乎没有影响。我们进一步鉴定了Spindlin1与核酸的关联,为其细胞周期调节及其他功能提供了生化基础。

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