蛋白质二硫键异构酶
生物化学
突变
蛋白质折叠
酵母
折叠(DSP实现)
化学
硫氧还蛋白
活动站点
定点突变
伴随蛋白
伴侣(临床)
生物
异构酶
酶
蛋白质工程
突变
基因
突变体
病理
工程类
电气工程
医学
作者
Robert B. Freedman,Timothy R. Hirst,Mick F. Tuite
标识
DOI:10.1016/0968-0004(94)90072-8
摘要
Protein disulphide isomerase (PDI) has been known for many years to assist in the folding of proteins containing disulphide bonds, but the exact mechanism by which it achieves this is only now becoming clear. The active site of PDI closely resembles that of the redox protein thioredoxin, and cDNA cloning has revealed a superfamily of proteins with related active-site sequences, in organisms ranging from bacteria to higher animals and plants. Recent mutagenesis studies are now helping to unravel the catalytic mechanism of PDI, and work in yeast and other systems is clarifying the physiological roles of the multiple PDI-related proteins.
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