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超稳定蛋白质的稳定性与折叠:眼晶状体晶状体蛋白及嗜热菌中的酶

Stability and folding of ultrastable proteins: eye lens crystallins and enzymes from thermophiles.

作者信息

Jaenicke R

机构信息

Institut für Biophysik und Physikalische Biochemie, Universität Regensburg, Germany.

出版信息

FASEB J. 1996 Jan;10(1):84-92. doi: 10.1096/fasebj.10.1.8566552.

Abstract

Soluble globular proteins exhibit marginal stabilities, equivalent to only a few weak intermolecular interactions. Extreme conditions in the biosphere, as well as acute physiological stress, require either mutative adaptation or stabilization by accessory proteins or extrinsic factors such as metabolites, cofactors, or compatible solvent components. No general strategies of stabilization have yet been established. However, certain contributions to stability have been elucidated by analyzing extremely stable proteins, such as crystallins from the eye lens, or proteins from hyperthermophilic microorganisms. Relating the structure and stability of homologous proteins from mesophiles and extremophiles, it becomes clear that stability increments may accumulate from 1) local interactions, 2) secondary or supersecondary structure, 3) packing and docking of domains, 4) association of subunits, and 5) conjugation with prosthetic groups, carbohydrate moieties, or nucleic acids, etc. Single and multiple point mutations, nicking and swapping of folding units in domain proteins, grafting of linker peptides between domains, and dissociation-reassociation of oligomeric proteins give insight into the cumulative nature of protein stability and its relation to the hierarchy of protein structure and folding. In this review, beta gamma-crystallins and enzymes from hyperthermophilic microorganisms are used as models to discuss mechanisms of protein stabilization.

摘要

可溶性球状蛋白表现出有限的稳定性,仅相当于少数微弱的分子间相互作用。生物圈中的极端条件以及急性生理应激,需要通过突变适应或由辅助蛋白或外在因素(如代谢物、辅因子或相容性溶剂成分)进行稳定。目前尚未建立普遍的稳定策略。然而,通过分析极其稳定的蛋白质,如眼晶状体中的晶状体蛋白或嗜热微生物中的蛋白质,已阐明了对稳定性的某些贡献。比较嗜温菌和嗜热菌同源蛋白的结构和稳定性,很明显稳定性的增加可能源于以下几个方面:1)局部相互作用;2)二级或超二级结构;3)结构域的堆积和对接;4)亚基的缔合;5)与辅基、碳水化合物部分或核酸等的结合。单点和多点突变、结构域蛋白折叠单元的切割和交换、结构域之间连接肽的嫁接以及寡聚蛋白的解离 - 重缔合,有助于深入了解蛋白质稳定性的累积性质及其与蛋白质结构和折叠层次的关系。在本综述中,以嗜热微生物中的βγ - 晶状体蛋白和酶为模型来讨论蛋白质稳定机制。

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