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Rhizonin生物合成分析揭示了多种环肽中药效团呋喃丙氨酸部分的起源。

Analysis of Rhizonin Biosynthesis Reveals Origin of Pharmacophoric Furylalanine Moieties in Diverse Cyclopeptides.

作者信息

Ehinger Friedrich J, Niehs Sarah P, Dose Benjamin, Dell Maria, Krabbe Jana, Pidot Sacha J, Stinear Timothy P, Scherlach Kirstin, Ross Claudia, Lackner Gerald, Hertweck Christian

机构信息

Department of Biomolecular Chemistry, Leibniz Institute for Natural Product Research and Infection Biology (HKI), Beutenbergstraße 11a, 07745, Jena, Germany.

Department of Microbiology and Immunology, Doherty Institute, 792 Elizabeth Street, Melbourne, 3000, Australia.

出版信息

Angew Chem Int Ed Engl. 2023 Oct 16;62(42):e202308540. doi: 10.1002/anie.202308540. Epub 2023 Sep 13.

Abstract

Rhizonin A and B are hepatotoxic cyclopeptides produced by bacterial endosymbionts (Mycetohabitans endofungorum) of the fungus Rhizopus microsporus. Their toxicity critically depends on the presence of 3-furylalanine (Fua) residues, which also occur in pharmaceutically relevant cyclopeptides of the endolide and bingchamide families. The biosynthesis and incorporation of Fua by non-ribosomal peptide synthetases (NRPS), however, has remained elusive. By genome sequencing and gene inactivation we elucidated the gene cluster responsible for rhizonin biosynthesis. A suite of isotope labeling experiments identified tyrosine and l-DOPA as Fua precursors and provided the first mechanistic insight. Bioinformatics, mutational analysis and heterologous reconstitution identified dioxygenase RhzB as necessary and sufficient for Fua formation. RhzB is a novel type of heme-dependent aromatic oxygenases (HDAO) that enabled the discovery of the bingchamide biosynthesis gene cluster through genome mining.

摘要

根霉毒素A和B是由微小根霉的细菌内共生体(内生真菌栖菌属)产生的具有肝毒性的环肽。它们的毒性关键取决于3-呋喃丙氨酸(Fua)残基的存在,这种残基也存在于内酰胺和柄茶酰胺家族与药物相关的环肽中。然而,非核糖体肽合成酶(NRPS)对Fua的生物合成和掺入仍不清楚。通过基因组测序和基因失活,我们阐明了负责根霉毒素生物合成的基因簇。一系列同位素标记实验确定酪氨酸和L-多巴是Fua的前体,并提供了首个作用机制方面的见解。生物信息学、突变分析和异源重组确定双加氧酶RhzB是Fua形成所必需且充分的。RhzB是一种新型的血红素依赖性芳香族加氧酶(HDAO),通过基因组挖掘,它使柄茶酰胺生物合成基因簇得以发现。

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