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2
A clinically relevant polymorphism in the Na/taurocholate cotransporting polypeptide (NTCP) occurs at a rheostat position.在胆盐共转运蛋白(NTCP)中存在一个临床相关的多态性,其位于变阻器位置。
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3
Substitutions at Nonconserved Rheostat Positions Modulate Function by Rewiring Long-Range, Dynamic Interactions.非保守变阻器位置的替换通过重新连接远程动态相互作用来调节功能。
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4
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8
The EMBL-EBI search and sequence analysis tools APIs in 2019.2019 年的 EMBL-EBI 搜索和序列分析工具 API。
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9
RheoScale: A tool to aggregate and quantify experimentally determined substitution outcomes for multiple variants at individual protein positions.RheoScale:一种工具,用于聚合和量化在单个蛋白质位置上多个变体的实验确定的替代结果。
Hum Mutat. 2018 Dec;39(12):1814-1826. doi: 10.1002/humu.23616. Epub 2018 Aug 28.
10
Computational predictors fail to identify amino acid substitution effects at rheostat positions.计算预测器无法识别变阻器位置处的氨基酸取代效应。
Sci Rep. 2017 Jan 30;7:41329. doi: 10.1038/srep41329.

在人醛缩酶 A 的变阻器位置进行取代会导致构象群体的转移。

Substitutions at a rheostat position in human aldolase A cause a shift in the conformational population.

机构信息

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

Department of Chemistry, University of Texas at San Antonio, San Antonio, Texas, USA.

出版信息

Protein Sci. 2022 Feb;31(2):357-370. doi: 10.1002/pro.4222. Epub 2021 Nov 12.

DOI:10.1002/pro.4222
PMID:34734672
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8819835/
Abstract

Some protein positions play special roles in determining the magnitude of protein function: at such "rheostat" positions, varied amino acid substitutions give rise to a continuum of functional outcomes, from wild type (or enhanced), to intermediate, to loss of function. This observed range raises interesting questions about the biophysical bases by which changes at single positions have such varied outcomes. Here, we assessed variants at position 98 in human aldolase A ("I98X"). Despite being ~17 Å from the active site and far from subunit interfaces, substitutions at position 98 have rheostatic contributions to the apparent cooperativity (n ) associated with fructose-1,6-bisphosphate substrate binding and moderately affected binding affinity. Next, we crystallized representative I98X variants to assess structural consequences. Residues smaller than the native isoleucine (cysteine and serine) were readily accommodated, and the larger phenylalanine caused only a slight separation of the two parallel helixes. However, the diffraction quality was reduced for I98F, and further reduced for I98Y. Intriguingly, the resolutions of the I98X structures correlated with their n values. We propose that substitution effects on both n and crystal lattice disruption arise from changes in the population of aldolase A conformations in solution. In combination with results computed for rheostat positions in other proteins, the results from this study suggest that rheostat positions accommodate a wide range of side chains and that structural consequences manifest as shifted ensemble populations and/or dynamics changes.

摘要

有些蛋白质位置在决定蛋白质功能的大小方面起着特殊作用

在这些“变阻器”位置,不同的氨基酸取代会产生功能结果的连续体,从野生型(或增强型)到中间型,再到功能丧失。这种观察到的范围提出了一个有趣的问题,即在单一位置的变化如何产生如此多样的结果。在这里,我们评估了人醛缩酶 A 中位置 98 的变体(“I98X”)。尽管距离活性位点约 17Å,且远离亚基界面,但位置 98 的取代对与果糖-1,6-二磷酸底物结合相关的表观协同性(n)具有变阻器贡献,并适度影响结合亲和力。接下来,我们结晶了代表性的 I98X 变体以评估结构后果。小于天然异亮氨酸(半胱氨酸和丝氨酸)的残基很容易被容纳,而较大的苯丙氨酸仅导致两条平行螺旋略微分离。然而,I98F 的衍射质量降低,而 I98Y 的衍射质量进一步降低。有趣的是,I98X 结构的分辨率与其 n 值相关。我们提出,n 值和晶体晶格破坏的取代效应都源于溶液中醛缩酶 A 构象的变化。结合其他蛋白质中变阻器位置的计算结果,本研究的结果表明,变阻器位置可容纳广泛的侧链,结构后果表现为偏移的整体种群和/或动力学变化。