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Identification of allosteric disulfides from labile bonds in X-ray structures

机译:从X射线结构中的不稳定键鉴定变构二硫键

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摘要

Protein disulfide bonds link pairs of cysteine sulfur atoms and are either structural or functional motifs. The allosteric disulfides control the function of the protein in which they reside when cleaved or formed. Here, we identify potential allosteric disulfides in all Protein Data Bank X-ray structures from bonds that are present in some molecules of a protein crystal but absent in others, or present in some structures of a protein but absent in others. We reasoned that the labile nature of these disulfides signifies a propensity for cleavage and so possible allosteric regulation of the protein in which the bond resides. A total of 511 labile disulfide bonds were identified. The labile disulfides are more stressed than the average bond, being characterized by high average torsional strain and stretching of the sulfur–sulfur bond and neighbouring bond angles. This pre-stress likely underpins their susceptibility to cleavage. The coagulation, complement and oxygen-sensing hypoxia inducible factor-1 pathways, which are known or have been suggested to be regulated by allosteric disulfides, are enriched in proteins containing labile disulfides. The identification of labile disulfide bonds will facilitate the study of this post-translational modification.
机译:蛋白质二硫键连接半胱氨酸硫原子对,是结构或功能性基元。当切割或形成时,变构二硫键控制它们所驻留的蛋白质的功能。在这里,我们从存在于蛋白质晶体的某些分子中但不存在于其他分子中,或存在于蛋白质的某些结构中但不存在于其他蛋白质中的键中识别出所有蛋白质数据库X射线结构中潜在的变构二硫键。我们认为这些二硫键的不稳定性质表明其易于裂解,因此可能存在对该键所处蛋白质的变构调节。总共鉴定出511个不稳定的二硫键。不稳定的二硫键比平均键承受更大的应力,其特征是平均扭应变高,硫-硫键和相邻键角的拉伸。这种预应力可能会增强它们对卵裂的敏感性。已知的或已建议由变构二硫化物调节的凝血,补体和氧敏感性低氧诱导因子-1途径富含含有不稳定二硫化物的蛋白质。不稳定的二硫键的鉴定将促进这种翻译后修饰的研究。

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