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真菌环脂肽苦孢菌素的生物合成,一种植物病原菌灰葡萄孢的新型选择性抑制剂。

Biosynthesis of the Fungal Cyclic Lipodepsipeptide Pleosporacin, a New Selective Inhibitor of the Phytopathogen Botrytis cinerea.

作者信息

Wieder Carsten, Wiechert Rainer, Yemelin Alexander, Sandjo Louis Pergaud, Thines Eckhard, Opatz Till, Schüffler Anja

机构信息

Institute of Molecular Physiology, Johannes Gutenberg-University, Hanns-Dieter-Hüsch Weg 17, 55128, Mainz, Germany.

Institut für Biotechnologie und Wirkstoff-Forschung gGmbH, Hanns-Dieter-Hüsch Weg 17, 55128, Mainz, Germany.

出版信息

Chembiochem. 2025 Jun 16;26(12):e202500315. doi: 10.1002/cbic.202500315. Epub 2025 May 23.

Abstract

Bioactivity-guided isolation led to the identification of the cyclic lipodepsipeptide pleosporacin (1) from the mycelia extract of fungal strain Pleosporales sp. IBWF 020-21, a potent selective inhibitor of the fungal phytopathogen Botrytis cinerea. The structure and stereochemistry of 1 were elucidated by NMR and Marfey analysis, respectively. Genome mining identified a candidate biosynthetic gene cluster encoding a hexamodular nonribosomal peptide synthetases, PleA, a fatty acyl-AMP ligase, PleB, and an aspartate decarboxylase, PleC. Reconstitution of pleABC allowed for heterologous production of 1 in Aspergillus oryzae and confirmed the identity of the ple cluster. Based on these findings a biosynthetic route is proposed, with PleB catalyzing lipoinitiation and PleC providing the nonproteinogenic amino acid β-alanine for the assembly of 1.

摘要

生物活性导向分离法从真菌菌株Pleosporales sp. IBWF 020 - 21的菌丝体提取物中鉴定出环状脂肽缩酚酸肽(1),它是真菌植物病原体灰葡萄孢的一种有效的选择性抑制剂。分别通过核磁共振(NMR)和马尔费伊分析阐明了1的结构和立体化学。基因组挖掘鉴定出一个候选生物合成基因簇,该基因簇编码一个六模块非核糖体肽合成酶PleA、一个脂肪酰-AMP连接酶PleB和一个天冬氨酸脱羧酶PleC。pleABC的重组使得在米曲霉中异源生产1成为可能,并确认了ple基因簇的身份。基于这些发现,提出了一条生物合成途径,其中PleB催化脂基起始,PleC为1的组装提供非蛋白质氨基酸β-丙氨酸。

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