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首页> 外文期刊>Angewandte Chemie >Probing the Catalytic Promiscuity of a Regio- and Stereospecific C-Glycosyltransferase from Mangifera indica
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Probing the Catalytic Promiscuity of a Regio- and Stereospecific C-Glycosyltransferase from Mangifera indica

机译:探测来自芒果的区域和立体特异性C-糖基转移酶的催化混杂性

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摘要

The catalytic promiscuity of the novel benzophenone C-glycosyltransferase, MiCGT, which is involved in the biosynthesis of mangiferin from Mangifera indica, was explored. MiCGT exhibited a robust capability to regio- and stereospecific C-glycosylation of 35 structurally diverse druglike scaffolds and simple phenolics with UDP-glucose, and also formed O- and N-glycosides. Moreover, MiCGT was able to generate C-xylosides with UDP-xylose. The OGT-reversibility of MiCGT was also exploited to generate C-glucosides with simple sugar donor. Three aryl-C-glycosides exhibited potent SGLT2 inhibitory activities with IC50 values of 2.6 x, 7.6 x, and 7.6 x 10(-7) M, respectively. These findings demonstrate for the first time the significant potential of an enzymatic approach to diversification through C-glycosidation of bioactive natural and unnatural products in drug discovery.
机译:探索了新型二苯甲酮C-糖基转移酶MiCGT的催化混杂性,该酶参与了印度芒果的芒果苷的生物合成。 MiCGT对35种结构多样的药物样支架和带有UDP-葡萄糖的简单酚类化合物具有较强的区域和立体特异性C-糖基化能力,还形成了O-和N-糖苷。此外,MiCGT能够与UDP木糖生成C-木糖苷。还利用MiCGT的OGT可逆性通过简单的糖供体生成C-葡萄糖苷。三个芳基-C-糖苷显示出强大的SGLT2抑制活性,IC50值分别为2.6 x,7.6 x和7.6 x 10(-7)M。这些发现首次证明了在药物开发中通过C-糖基化生物活性天然和非天然产物的酶促方法多样化的巨大潜力。

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