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车前草多底物还原酶:在短链还原酶超家族中的结构与功能。

A multisubstrate reductase from Plantago major: structure-function in the short chain reductase superfamily.

机构信息

European Synchrotron Radiation Facility, Structural Biology Group, 71 Avenue des Martyrs, F-38000, Grenoble, France.

Department of Chemistry, Syracuse University, Syracuse, NY, 13244, USA.

出版信息

Sci Rep. 2018 Oct 4;8(1):14796. doi: 10.1038/s41598-018-32967-1.

Abstract

The short chain dehydrogenase/reductase superfamily (SDR) is a large family of NAD(P)H-dependent enzymes found in all kingdoms of life. SDRs are particularly well-represented in plants, playing diverse roles in both primary and secondary metabolism. In addition, some plant SDRs are also able to catalyse a reductive cyclisation reaction critical for the biosynthesis of the iridoid backbone that contains a fused 5 and 6-membered ring scaffold. Mining the EST database of Plantago major, a medicinal plant that makes iridoids, we identified a putative 5β-progesterone reductase gene, PmMOR (P. major multisubstrate oxido-reductase), that is 60% identical to the iridoid synthase gene from Catharanthus roseus. The PmMOR protein was recombinantly expressed and its enzymatic activity assayed against three putative substrates, 8-oxogeranial, citral and progesterone. The enzyme demonstrated promiscuous enzymatic activity and was able to not only reduce progesterone and citral, but also to catalyse the reductive cyclisation of 8-oxogeranial. The crystal structures of PmMOR wild type and PmMOR mutants in complex with NADP or NAD and either 8-oxogeranial, citral or progesterone help to reveal the substrate specificity determinants and catalytic machinery of the protein. Site-directed mutagenesis studies were performed and provide a foundation for understanding the promiscuous activity of the enzyme.

摘要

短链脱氢酶/还原酶超家族(SDR)是一个庞大的 NAD(P)H 依赖酶家族,存在于所有生命领域。SDR 在植物中尤为丰富,在初级和次级代谢中发挥着多样化的作用。此外,一些植物 SDR 还能够催化还原环化反应,这对于含融合的 5 元和 6 元环骨架的裂环环烯醚萜的生物合成至关重要。在挖掘药用植物车前草的 EST 数据库时,我们鉴定出一个假定的 5β-孕烯醇酮还原酶基因 PmMOR(车前草多底物氧化还原酶),它与长春花中的裂环环烯醚萜合酶基因有 60%的同源性。PmMOR 蛋白被重组表达,并针对三种假定的底物 8-氧香叶醛、柠檬醛和孕酮进行了酶活性测定。该酶表现出混杂的酶活性,不仅能够还原孕酮和柠檬醛,还能够催化 8-氧香叶醛的还原环化。PmMOR 野生型和 PmMOR 突变体与 NADP 或 NAD 以及 8-氧香叶醛、柠檬醛或孕酮复合物的晶体结构有助于揭示该蛋白的底物特异性决定因素和催化机制。进行了定点突变研究,为理解该酶的混杂活性提供了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/93d7/6172241/4711f10f7100/41598_2018_32967_Fig1_HTML.jpg

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