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工程化的 Sortases 在肽和蛋白质化学中的应用。

Engineered Sortases in Peptide and Protein Chemistry.

机构信息

Freie Universität Berlin, Institute of Chemistry and Biochemistry, Thielallee 63, 14195, Berlin, Germany.

University of Tübingen, Interfaculty Institute of Biochemistry (IFIB), Auf der Morgenstelle 34, 72076, Tübingen, Germany.

出版信息

Chembiochem. 2021 Apr 16;22(8):1347-1356. doi: 10.1002/cbic.202000745. Epub 2021 Feb 3.

Abstract

The transpeptidase sortase A of Staphylococcus aureus (Sa-SrtA) is a valuable tool in protein chemistry. The native enzyme anchors surface proteins containing a highly conserved LPxTG sorting motif to a terminal glycine residue of the peptidoglycan layer in Gram-positive bacteria. This reaction is exploited for sortase-mediated ligation (SML), allowing the site-specific linkage of synthetic peptides and recombinant proteins by a native peptide bond. However, the moderate catalytic efficiency and specificity of Sa-SrtA fueled the development of new biocatalysts for SML, including the screening of sortase A variants form microorganisms other than S. aureus and the directed protein evolution of the Sa-SrtA enzyme itself. Novel display platforms and screening formats were developed to isolate sortases with altered properties from mutant libraries. This yielded sortases with strongly enhanced catalytic activity and enzymes recognizing new sorting motifs as substrates. This minireview focuses on recent advances in the field of directed sortase evolution and applications of these tailor-made enzymes in biochemistry.

摘要

金黄色葡萄球菌(Sa-SrtA)转肽酶 SrtA 在蛋白质化学领域是一种很有价值的工具。天然酶将含有高度保守 LPxTG 分拣基序的表面蛋白锚定到革兰氏阳性菌肽聚糖层的末端甘氨酸残基上。该反应被用于转肽酶介导的连接(SML),允许通过天然肽键对合成肽和重组蛋白进行特异性连接。然而,Sa-SrtA 的中等催化效率和特异性促使人们开发了用于 SML 的新型生物催化剂,包括筛选来自金黄色葡萄球菌以外的微生物的 SrtA 变体,以及对 Sa-SrtA 酶本身进行定向蛋白质进化。新的展示平台和筛选格式被开发出来,以从突变文库中分离具有改变特性的转肽酶。这产生了具有强烈增强的催化活性的转肽酶,以及能够识别新分拣基序作为底物的酶。这篇迷你综述重点介绍了定向转肽酶进化领域的最新进展,以及这些定制酶在生物化学中的应用。

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