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蛋白质超家族的物理起源

Physical origins of protein superfamilies.

作者信息

Zeldovich Konstantin B, Berezovsky Igor N, Shakhnovich Eugene I

机构信息

Department of Chemistry and Chemical Biology, Harvard University, 12 Oxford Street, Cambridge, MA 02138, USA.

出版信息

J Mol Biol. 2006 Apr 7;357(4):1335-43. doi: 10.1016/j.jmb.2006.01.081. Epub 2006 Feb 6.

Abstract

In this work, we discovered a fundamental connection between selection for protein stability and emergence of preferred structures of proteins. Using a standard exact three-dimensional lattice model we evolve sequences starting from random ones and determine the exact native structure after each mutation. Acceptance of mutations is biased to select for stable proteins. We found that certain structures, "wonderfolds", are independently discovered numerous times as native states of stable proteins in many unrelated runs of selection. The strong dependence of lattice fold usage on the structural determinant of designability quantitatively reproduces uneven fold usage in natural proteins. Diversity of sequences that fold into wonderfold structures gives rise to superfamilies, i.e. sets of dissimilar sequences that fold into the same or very similar structures. The present work establishes a model of pre-biotic structure selection, which identifies dominant structural patterns emerging upon optimization of proteins for survival in a hot environment. Convergently discovered pre-biotic initial superfamilies with wonderfold structures could have served as a seed for subsequent biological evolution involving gene duplications and divergence.

摘要

在这项工作中,我们发现了蛋白质稳定性选择与蛋白质优选结构出现之间的基本联系。使用标准的精确三维晶格模型,我们从随机序列开始演化序列,并在每次突变后确定精确的天然结构。突变的接受偏向于选择稳定的蛋白质。我们发现,某些结构,即“奇妙折叠”,在许多不相关的选择过程中作为稳定蛋白质的天然状态被多次独立发现。晶格折叠使用对可设计性结构决定因素的强烈依赖性定量地再现了天然蛋白质中不均匀的折叠使用情况。折叠成奇妙折叠结构的序列多样性产生了超家族,即折叠成相同或非常相似结构的不同序列集合。目前这项工作建立了一个前生物结构选择模型,该模型确定了在热环境中为生存而优化蛋白质时出现的主导结构模式。具有奇妙折叠结构的趋同发现的前生物初始超家族可能作为随后涉及基因复制和分化的生物进化种子。

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