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靶向昆虫谷氨酸门控氯离子通道的奥卡胺生物合成及结构-活性关系研究。

Biosynthesis and Structure-Activity Relationship Studies of Okaramines That Target Insect Glutamate-Gated Chloride Channels.

机构信息

Natural Product Biosynthesis Research Unit , RIKEN Center for Sustainable Resource Science , Wako , Saitama 351-0198 , Japan.

Department of Applied Biological Chemistry, Faculty of Agriculture , Kindai University , Nara , Nara 631-8505 , Japan.

出版信息

ACS Chem Biol. 2018 Mar 16;13(3):561-566. doi: 10.1021/acschembio.7b00878. Epub 2018 Feb 2.

Abstract

Prenylated indole alkaloid okaramines selectively target insect glutamate-gated chloride channels (GluCls). Because of their highly complex structures, including azocine and azetidine rings, total synthesis of okaramine A or B has not been achieved, preventing evaluation of the biological activities of okaramines. Biosynthetic approaches provide alternatives to accessing structurally diverse derivatives and enabling the elucidation of structure-activity relationships. To explore the biosynthetic potential of okaramines, gene knockout experiments of an okaramine-producer fungus were performed. The deletion mutants of the oxygenase genes okaB, okaD, okaE, and okaG provided analogues that were unlikely to be accumulated in the normal biosynthetic process of the wild-type strain. Analysis of the structure-activity relationships of okaramines collected from the fungal cultures revealed that 1,4-dihydroazocine and N-aliphatic group attached to the indole were crucial for GluCl-activating activity. This provided insights into further derivatization of the complex structure of okaramines in order to facilitate the development of new insecticides.

摘要

烯丙基吲哚生物碱奥卡胺选择性靶向昆虫谷氨酸门控氯离子通道(GluCls)。由于其高度复杂的结构,包括氮杂环辛烷和氮杂环丁烷环,奥卡胺 A 或 B 的全合成尚未实现,这阻碍了对奥卡胺生物活性的评估。生物合成方法为获得结构多样的衍生物提供了替代方法,并能够阐明结构-活性关系。为了探索奥卡胺的生物合成潜力,对奥卡胺产生菌进行了基因敲除实验。氧合酶基因 okaB、okaD、okaE 和 okaG 的缺失突变体提供了类似物,这些类似物不太可能在野生型菌株的正常生物合成过程中积累。从真菌培养物中收集的奥卡胺的结构-活性关系分析表明,1,4-二氢氮杂环辛烷和连接到吲哚的 N-脂族基团对于 GluCl 激活活性至关重要。这为进一步衍生奥卡胺的复杂结构提供了思路,以促进新型杀虫剂的开发。

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