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Est3 的结构揭示了一种双峰表面,在端粒复制中具有不同的作用。

Structure of Est3 reveals a bimodal surface with differential roles in telomere replication.

机构信息

Department of Chemistry and Biochemistry, University of Colorado Boulder, Boulder, CO 80309-0596.

出版信息

Proc Natl Acad Sci U S A. 2014 Jan 7;111(1):214-8. doi: 10.1073/pnas.1316453111. Epub 2013 Dec 16.

Abstract

Telomerase is essential for continuous cellular proliferation. Substantial insights have come from studies of budding yeast telomerase, which consists of a catalytic core in association with two regulatory proteins, ever shorter telomeres 1 and 3 (Est1 and Est3). We report here a high-resolution structure of the Est3 telomerase subunit determined using a recently developed strategy that combines minimal NMR experimental data with Rosetta de novo structure prediction algorithms. Est3 adopts an overall protein fold which is structurally similar to that adopted by the shelterin component TPP1. However, the characteristics of the surface of the experimentally determined Est3 structure are substantially different from those predicted by prior homology-based models of Est3. Structure-guided mutagenesis of the complete surface of the Est3 protein reveals two adjacent patches on a noncanonical face of the protein that differentially mediate telomere function. Mapping these two patches on the Est3 structure defines a set of shared features between Est3 and HsTPP1, suggesting an analogous multifunctional surface on TPP1.

摘要

端粒酶对于细胞的持续增殖是必不可少的。芽殖酵母端粒酶的研究提供了大量的认识,它由一个催化核心与两个调节蛋白组成,即越来越短的端粒 1 和 3(Est1 和 Est3)。我们在这里报告了使用最近开发的策略确定的 Est3 端粒酶亚基的高分辨率结构,该策略结合了最小的 NMR 实验数据和 Rosetta 从头结构预测算法。Est3 采用了一种整体蛋白质折叠结构,在结构上与庇护素成分 TPP1 相似。然而,实验确定的 Est3 结构表面的特征与之前基于同源性的 Est3 模型预测的特征有很大的不同。对 Est3 蛋白完整表面进行结构引导的诱变揭示了蛋白质非典型面上两个相邻的斑块,它们以不同的方式介导端粒功能。将这两个斑块映射到 Est3 结构上,定义了 Est3 和 HsTPP1 之间的一组共享特征,表明 TPP1 上存在类似的多功能表面。

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