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发现参与抗糖尿病植物代谢物蒙布列汀 A 生物合成的 UDP-糖基转移酶和 BAHD-酰基转移酶。

Discovery of UDP-Glycosyltransferases and BAHD-Acyltransferases Involved in the Biosynthesis of the Antidiabetic Plant Metabolite Montbretin A.

机构信息

Michael Smith Laboratories, University of British Columbia, Vancouver BC V6T 1Z4, Canada.

Department of Botany, University of British Columbia, Vancouver BC V6T 1Z4, Canada.

出版信息

Plant Cell. 2018 Aug;30(8):1864-1886. doi: 10.1105/tpc.18.00406. Epub 2018 Jul 2.

Abstract

Plant specialized metabolism serves as a rich resource of biologically active molecules for drug discovery. The acylated flavonol glycoside montbretin A (MbA) and its precursor myricetin 3--(6'--caffeoyl)-glucosyl rhamnoside (mini-MbA) are potent inhibitors of human pancreatic α-amylase and are being developed as drug candidates to treat type-2 diabetes. MbA occurs in corms of the ornamental plant montbretia (), but a system for large-scale MbA production is currently unavailable. Biosynthesis of MbA from the flavonol myricetin and MbA accumulation occur during early stages of corm development. We established myricetin 3--rhamnoside (MR), myricetin 3--glucosyl rhamnoside (MRG), and mini-MbA as the first three intermediates of MbA biosynthesis. Contrasting the transcriptomes of young and old corms revealed differentially expressed UDP-sugar-dependent glycosyltransferases (UGTs) and BAHD-acyltransferases (BAHD-ATs). UGT77B2 and UGT709G2 catalyze the consecutive glycosylation of myricetin to produce MR and of MR to give MRG, respectively. In addition, two BAHD-ATs, CcAT1 and CcAT2, catalyze the acylation of MRG to complete the formation of mini-MbA. Transcript profiles of UGT77B2, UGT709G2, CcAT1, and CcAT2 during corm development matched the metabolite profile of MbA accumulation. Expression of these enzymes in wild tobacco () resulted in the formation of a surrogate mini-MbA, validating the potential for metabolic engineering of mini-MbA in a heterologous plant system.

摘要

植物特化代谢为药物发现提供了丰富的生物活性分子资源。酰化黄酮醇糖苷蒙布替林 A(MbA)及其前体杨梅素 3--(6'--咖啡酰)-葡萄糖基鼠李糖苷(迷你-MbA)是有效的人胰腺α-淀粉酶抑制剂,目前正在被开发为治疗 2 型糖尿病的候选药物。MbA 存在于观赏植物鹤望兰()的球茎中,但目前尚无大规模生产 MbA 的系统。MbA 是从黄酮醇杨梅素生物合成的,MbA 的积累发生在球茎发育的早期阶段。我们确立了杨梅素 3--鼠李糖苷(MR)、杨梅素 3--葡萄糖基鼠李糖苷(MRG)和迷你-MbA 作为 MbA 生物合成的前三个中间体。比较幼龄和老龄球茎的转录组,揭示了差异表达的 UDP-糖依赖性糖基转移酶(UGTs)和 BAHD-酰基转移酶(BAHD-AT)。UGT77B2 和 UGT709G2 分别催化杨梅素的连续糖基化生成 MR 和 MR 生成 MRG。此外,两种 BAHD-ATs,CcAT1 和 CcAT2,催化 MRG 的酰化完成迷你-MbA 的形成。UGT77B2、UGT709G2、CcAT1 和 CcAT2 在球茎发育过程中的转录谱与 MbA 积累的代谢物谱相匹配。这些酶在野生烟草()中的表达导致了替代迷你-MbA 的形成,验证了在异源植物系统中对迷你-MbA 进行代谢工程的潜力。

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