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基于结构的哺乳动物糖基转移酶机制和底物特异性的诱变分析:猪 ST3Gal-I。

Structure-based mutagenic analysis of mechanism and substrate specificity in mammalian glycosyltransferases: porcine ST3Gal-I.

机构信息

Department of Chemistry, University of British Columbia, Vancouver, BC, Canada.

出版信息

Glycobiology. 2013 May;23(5):536-45. doi: 10.1093/glycob/cwt001. Epub 2013 Jan 8.

Abstract

Sialyltransferases (STs) play essential roles in signaling and in the cellular recognition processes of mammalian cells by selectively installing cell-surface sialic acids in an appropriate manner both temporally and organ-specifically. The availability of the first three-dimensional structure of a mammalian (GT29) sialyltransferase has, for the first time, allowed quantitative structure/function analyses to be performed, thereby providing reliable insights into the roles of key active site amino acids. Kinetic analyses of mutants of ST3Gal-I, in conjunction with structural studies, have confirmed the mechanistic roles of His302 and His319 as general acid and base catalysts, respectively, and have quantitated other interactions with the cytosine monophosphate-N-acetyl β-neuraminic acid donor substrate. The contributions of side chains that provide key interactions with the acceptor substrate, defining its specificity, have also been quantitated. Particularly important transition-state interactions of 2.5 and 2.7 kcal mol(-1) are found between the acceptor axial 4-hydroxyl and the conserved side chains of Gln108 and Tyr269, respectively. These results provide a basis for the engineering of mammalian STs to accommodate non-natural substrate analogs that should prove valuable as chemical biological probes of sialyltransferase function.

摘要

唾液酸转移酶(STs)通过选择性地在时间和组织特异性上以适当的方式在细胞表面安装唾液酸,在哺乳动物细胞的信号转导和细胞识别过程中发挥重要作用。第一个哺乳动物(GT29)唾液酸转移酶的三维结构的出现,首次允许进行定量结构/功能分析,从而为关键活性位点氨基酸的作用提供了可靠的见解。ST3Gal-I 突变体的动力学分析与结构研究相结合,证实了 His302 和 His319 分别作为广义酸和碱催化剂的作用,并量化了与胞苷单磷酸-N-乙酰 β-神经氨酸供体底物的其他相互作用。还量化了与受体底物提供关键相互作用、定义其特异性的侧链的贡献。在 2.5 和 2.7 kcal mol(-1) 之间发现了与受体轴向 4-羟基和保守侧链 Gln108 和 Tyr269 之间的特别重要的过渡态相互作用。这些结果为工程改造哺乳动物 ST 以适应非天然底物类似物提供了基础,这些类似物应该作为唾液酸转移酶功能的化学生物学探针很有价值。

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