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糖皮质激素受体进化中的历史偶然性及其生物物理基础。

Historical contingency and its biophysical basis in glucocorticoid receptor evolution.

机构信息

1] Institute of Molecular Biology and Department of Chemistry &Biochemistry, University of Oregon, Eugene, Oregon 97403, USA [2] Departments of Human Genetics and Ecology &Evolution, University of Chicago, Chicago, Illinois 60637, USA.

1] Departments of Human Genetics and Ecology &Evolution, University of Chicago, Chicago, Illinois 60637, USA [2] Institute of Ecology and Evolution, University of Oregon, Eugene, Oregon 97403, USA.

出版信息

Nature. 2014 Aug 14;512(7513):203-7. doi: 10.1038/nature13410. Epub 2014 Jun 15.

Abstract

Understanding how chance historical events shape evolutionary processes is a central goal of evolutionary biology. Direct insights into the extent and causes of evolutionary contingency have been limited to experimental systems, because it is difficult to know what happened in the deep past and to characterize other paths that evolution could have followed. Here we combine ancestral protein reconstruction, directed evolution and biophysical analysis to explore alternative 'might-have-been' trajectories during the ancient evolution of a novel protein function. We previously found that the evolution of cortisol specificity in the ancestral glucocorticoid receptor (GR) was contingent on permissive substitutions, which had no apparent effect on receptor function but were necessary for GR to tolerate the large-effect mutations that caused the shift in specificity. Here we show that alternative mutations that could have permitted the historical function-switching substitutions are extremely rare in the ensemble of genotypes accessible to the ancestral GR. In a library of thousands of variants of the ancestral protein, we recovered historical permissive substitutions but no alternative permissive genotypes. Using biophysical analysis, we found that permissive mutations must satisfy at least three physical requirements--they must stabilize specific local elements of the protein structure, maintain the correct energetic balance between functional conformations, and be compatible with the ancestral and derived structures--thus revealing why permissive mutations are rare. These findings demonstrate that GR evolution depended strongly on improbable, non-deterministic events, and this contingency arose from intrinsic biophysical properties of the protein.

摘要

理解偶然历史事件如何塑造进化过程是进化生物学的一个核心目标。直接了解进化偶然性的程度和原因仅限于实验系统,因为很难知道过去发生了什么,也很难描述进化可能遵循的其他途径。在这里,我们结合祖先蛋白重建、定向进化和生物物理分析,来探索在新型蛋白功能的古老进化过程中替代的“可能发生的”轨迹。我们之前发现,皮质醇特异性在祖先糖皮质激素受体(GR)中的进化是偶然的,这取决于允许性取代,这些取代对受体功能没有明显影响,但对于 GR 容忍引起特异性转变的大效应突变是必要的。在这里,我们表明,在祖先 GR 可获得的基因型集合中,允许历史功能转换取代的替代突变极其罕见。在数千个祖先蛋白变体的文库中,我们恢复了历史允许取代,但没有其他允许的基因型。通过生物物理分析,我们发现允许性突变必须满足至少三个物理要求——它们必须稳定蛋白结构的特定局部元素,维持功能构象之间正确的能量平衡,并且与祖先和衍生结构兼容——从而揭示了为什么允许性突变是罕见的。这些发现表明,GR 的进化强烈依赖于偶然的、非确定性的事件,这种偶然性源自于蛋白的内在物理特性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b91d/4447330/a9b59ca4225a/nihms590618f1.jpg

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