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当替换发生在与物种形成分歧的非保守位置时,变阻器功能结果就会出现。

Rheostat functional outcomes occur when substitutions are introduced at nonconserved positions that diverge with speciation.

机构信息

Department of Biochemistry and Molecular Biology, The University of Kansas Medical Center, Kansas City, Kansas, USA.

Department of Biochemistry and Cell Biology, Geisel School of Medicine at Dartmouth College, Hanover, New Hampshire, USA.

出版信息

Protein Sci. 2021 Sep;30(9):1833-1853. doi: 10.1002/pro.4136. Epub 2021 Jun 11.

Abstract

When amino acids vary during evolution, the outcome can be functionally neutral or biologically-important. We previously found that substituting a subset of nonconserved positions, "rheostat" positions, can have surprising effects on protein function. Since changes at rheostat positions can facilitate functional evolution or cause disease, more examples are needed to understand their unique biophysical characteristics. Here, we explored whether "phylogenetic" patterns of change in multiple sequence alignments (such as positions with subfamily specific conservation) predict the locations of functional rheostat positions. To that end, we experimentally tested eight phylogenetic positions in human liver pyruvate kinase (hLPYK), using 10-15 substitutions per position and biochemical assays that yielded five functional parameters. Five positions were strongly rheostatic and three were non-neutral. To test the corollary that positions with low phylogenetic scores were not rheostat positions, we combined these phylogenetic positions with previously-identified hLPYK rheostat, "toggle" (most substitution abolished function), and "neutral" (all substitutions were like wild-type) positions. Despite representing 428 variants, this set of 33 positions was poorly statistically powered. Thus, we turned to the in vivo phenotypic dataset for E. coli lactose repressor protein (LacI), which comprised 12-13 substitutions at 329 positions and could be used to identify rheostat, toggle, and neutral positions. Combined hLPYK and LacI results show that positions with strong phylogenetic patterns of change are more likely to exhibit rheostat substitution outcomes than neutral or toggle outcomes. Furthermore, phylogenetic patterns were more successful at identifying rheostat positions than were co-evolutionary or eigenvector centrality measures of evolutionary change.

摘要

当氨基酸在进化过程中发生变化时,结果可能是功能上的中性或生物学上的重要。我们之前发现,取代一组非保守的位置,“变阻器”位置,可以对蛋白质功能产生惊人的影响。由于变阻器位置的变化可以促进功能进化或导致疾病,因此需要更多的例子来了解它们独特的生物物理特性。在这里,我们探讨了多序列比对中变化的“系统发育”模式(例如具有亚家族特异性保守性的位置)是否可以预测功能变阻器位置的位置。为此,我们使用每个位置 10-15 个取代实验测试了人肝丙酮酸激酶(hLPYK)中的八个系统发育位置,并进行了生化测定,得出了五个功能参数。五个位置是强烈的变阻器,三个是非中性的。为了测试位置的系统发育得分低不是变阻器位置的推论,我们将这些系统发育位置与之前鉴定的 hLPYK 变阻器、“拨动”(大多数取代都破坏了功能)和“中性”(所有取代都与野生型相同)位置结合起来。尽管代表了 428 个变体,但这组 33 个位置的统计能力很差。因此,我们转向了大肠杆菌乳糖阻遏蛋白(LacI)的体内表型数据集,该数据集包含 329 个位置的 12-13 个取代,可以用于识别变阻器、拨动和中性位置。hLPYK 和 LacI 的综合结果表明,变化的系统发育模式较强的位置比中性或拨动结果更有可能表现出变阻器取代的结果。此外,与进化变化的共进化或特征向量中心性度量相比,系统发育模式更成功地识别了变阻器位置。

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