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原位分析蛋白质组热稳定的渗透物机制。

In situ analysis of osmolyte mechanisms of proteome thermal stabilization.

机构信息

Department of Biology, Institute of Molecular Systems Biology, ETH Zurich, Zurich, Switzerland.

Division of Computational Genomics and Systems Genetics, German Cancer Research Center (DKFZ), Heidelberg, Germany.

出版信息

Nat Chem Biol. 2024 Aug;20(8):1053-1065. doi: 10.1038/s41589-024-01568-7. Epub 2024 Feb 29.

Abstract

Organisms use organic molecules called osmolytes to adapt to environmental conditions. In vitro studies indicate that osmolytes thermally stabilize proteins, but mechanisms are controversial, and systematic studies within the cellular milieu are lacking. We analyzed Escherichia coli and human protein thermal stabilization by osmolytes in situ and across the proteome. Using structural proteomics, we probed osmolyte effects on protein thermal stability, structure and aggregation, revealing common mechanisms but also osmolyte- and protein-specific effects. All tested osmolytes (trimethylamine N-oxide, betaine, glycerol, proline, trehalose and glucose) stabilized many proteins, predominantly via a preferential exclusion mechanism, and caused an upward shift in temperatures at which most proteins aggregated. Thermal profiling of the human proteome provided evidence for intrinsic disorder in situ but also identified potential structure in predicted disordered regions. Our analysis provides mechanistic insight into osmolyte function within a complex biological matrix and sheds light on the in situ prevalence of intrinsically disordered regions.

摘要

生物体利用称为渗透物的有机分子来适应环境条件。体外研究表明,渗透物使蛋白质热稳定,但机制存在争议,并且缺乏细胞环境内的系统研究。我们在原位和整个蛋白质组水平上分析了渗透物对大肠杆菌和人类蛋白质的热稳定性的影响。使用结构蛋白质组学,我们探测了渗透物对蛋白质热稳定性、结构和聚集的影响,揭示了共同的机制,但也揭示了渗透物和蛋白质特异性的影响。所有测试的渗透物(氧化三甲胺、甜菜碱、甘油、脯氨酸、海藻糖和葡萄糖)都稳定了许多蛋白质,主要通过优先排斥机制,并且导致大多数蛋白质聚集的温度升高。对人类蛋白质组的热分析提供了原位固有无序的证据,但也确定了预测无序区域中的潜在结构。我们的分析为复杂生物基质中渗透物功能提供了机制上的见解,并阐明了固有无序区域在原位的普遍存在。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fd0d/11288892/204b0f2d8c00/41589_2024_1568_Fig1_HTML.jpg

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