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选择性 1 H NMR 方法揭示了在无序蛋白质中具有功能相关性的脯氨酸顺/反异构体:次要形式的特征、磷酸化的影响以及在蛋白质组中的存在。

Selective H NMR Methods Reveal Functionally Relevant Proline cis/trans Isomers in Intrinsically Disordered Proteins: Characterization of Minor Forms, Effects of Phosphorylation, and Occurrence in Proteome.

机构信息

Eötvös Loránd University, Institute of Chemistry, Pázmány Péter s. 1/a, 1117, Budapest, Hungary.

Semmelweis University, Doctoral School of Pharmaceutical Sciences, Üllői út 26, 1085, Budapest, Hungary.

出版信息

Angew Chem Int Ed Engl. 2022 Jan 3;61(1):e202108361. doi: 10.1002/anie.202108361. Epub 2021 Nov 16.

Abstract

It is important to identify proline cis/trans isomers that appear in several regulatory mechanisms of proteins, and to characterize minor species that are present due to the conformational heterogeneity in intrinsically disordered proteins (IDPs). To obtain residue level information on these mobile systems we introduce two H -detected, proline selective, real-time homodecoupled NMR experiments and analyze the proline abundant transactivation domain of p53. The measurements are sensitive enough to identify minor conformers present in 4-15 % amounts; moreover, we show the consequences of CK2 phosphorylation on the cis/trans-proline equilibrium. Using our results and available literature data we perform a statistical analysis on how the amino acid type effects the cis/trans-proline distribution. The methods are applicable under physiological conditions, they can contribute to find key proline isomers in proteins, and statistical analysis results may help in amino acid sequence optimization for biotechnological purposes.

摘要

鉴定出几种蛋白质调控机制中出现的脯氨酸顺/反异构体,并对由于无序蛋白质(IDP)构象异质性而存在的少量物种进行特征描述,这一点很重要。为了获得有关这些可移动系统的残基水平信息,我们引入了两种 H 检测、脯氨酸选择性、实时同核去耦 NMR 实验,并对 p53 的脯氨酸丰富的转录激活结构域进行了分析。这些测量的灵敏度足以识别存在于 4-15% 量中的少量构象;此外,我们还展示了 CK2 磷酸化对顺/反式脯氨酸平衡的影响。使用我们的结果和可用的文献数据,我们对氨基酸类型如何影响顺/反式脯氨酸分布进行了统计分析。这些方法适用于生理条件下,可以帮助找到蛋白质中的关键脯氨酸异构体,并且统计分析结果可能有助于针对生物技术目的进行氨基酸序列优化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f9cd/9299183/67bab993ef3c/ANIE-61-0-g005.jpg

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