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Diverse sequences are functional at the C-terminus of the E. coll peripiasmic chaperone SurA

机译:不同序列在大肠杆菌周围型伴侣SurA的C-末端起作用

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SurA is a major peripiasmic molecular chaperone in Escherichia coli and has been shown to assist the biogenesis of several outer membrane proteins. The C-terminal fragment of SurA folds into a short p-strand, which forms a small three-stranded anti-parallel p-sheet module with the N-terminal beta-hairpin. We found that the length of the C-terminal fragment, rather than its exact amino acid composition, had a big impact on SurA function. To investigate the determinant factor of the C-terminal sequence, we created a library of SurA constructs randomized in the last 10 residues. We screened the library and randomly analyzed 19 constructs that displayed SurA activity. The C-termini of these constructs shared little sequence similarity, except that p-strand-forming residues were preferentially enriched. Three SurA constructs were expressed and purified for structural characterization. Circular di-chroism and fluorescence spectroscopy analyses revealed that their structures were similar to the structure of the wild-type SurA. Our results suggest that for scaffolding purpose proteins may tolerate various sequences provided certain general requirements such as hydrophobicity and secondary structure propensity are satisfied. Furthermore, the sequence tolerance of SurA at the C-terminus indicates that this area is not likely to be involved in substrate binding.
机译:SurA是大肠杆菌中主要的围生性分子伴侣,已被证明可协助多种外膜蛋白的生物发生。 SurA的C端片段折叠成一条短的p链,与N端β-发夹形成一个小的三链反平行p-sheet模块。我们发现,C末端片段的长度,而不是其确切的氨基酸组成,对SurA功能有很大的影响。为了研究C末端序列的决定因素,我们创建了一个在最近10个残基中随机分配的SurA构建体文库。我们筛选了文库并随机分析了显示SurA活性的19个构建体。这些构建体的C末端几乎没有序列相似性,只是优先富集了形成p链的残基。表达并纯化了三种SurA构建体以进行结构表征。圆二色性和荧光光谱分析表明,它们的结构与野生型SurA的结构相似。我们的结果表明,出于支架目的,只要满足某些一般性要求(如疏水性和二级结构倾向),蛋白质就可以耐受各种序列。此外,SurA在C端的序列耐受性表明该区域不太可能参与底物结合。

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