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海纳酰胺 A1-A3 和 B1-B5 的结构与生物合成,它们是拉沙菌素脂肽族中的抗真菌成员。

The structure and biosynthesis of heinamides A1-A3 and B1-B5, antifungal members of the laxaphycin lipopeptide family.

机构信息

Department of Microbiology, Faculty of Agriculture and Forestry, University of Helsinki, Helsinki, Finland.

Department of Chemistry, University of Jyväskylä, Jyväskylä, Finland and Department of Biological and Environmental Science, Nanoscience Center, University of Jyväskylä, Jyväskylä, Finland.

出版信息

Org Biomol Chem. 2021 Jun 30;19(25):5577-5588. doi: 10.1039/d1ob00772f.

DOI:10.1039/d1ob00772f
PMID:34085692
Abstract

Laxaphycins are a family of cyclic lipopeptides with synergistic antifungal and antiproliferative activities. They are produced by multiple cyanobacterial genera and comprise two sets of structurally unrelated 11- and 12-residue macrocyclic lipopeptides. Here, we report the discovery of new antifungal laxaphycins from Nostoc sp. UHCC 0702, which we name heinamides, through antimicrobial bioactivity screening. We characterized the chemical structures of eight heinamide structural variants A1-A3 and B1-B5. These variants contain the rare non-proteinogenic amino acids 3-hydroxy-4-methylproline, 4-hydroxyproline, 3-hydroxy-d-leucine, dehydrobutyrine, 5-hydroxyl β-amino octanoic acid, and O-carbamoyl-homoserine. We obtained an 8.6-Mb complete genome sequence from Nostoc sp. UHCC 0702 and identified the 93 kb heinamide biosynthetic gene cluster. The structurally distinct heinamides A1-A3 and B1-B5 variants are synthesized using an unusual branching biosynthetic pathway. The heinamide biosynthetic pathway also encodes several enzymes that supply non-proteinogenic amino acids to the heinamide synthetase. Through heterologous expression, we showed that (2S,4R)-4-hydroxy-l-proline is supplied through the action of a novel enzyme LxaN, which hydroxylates l-proline. 11- and 12-residue heinamides have the characteristic synergistic activity of laxaphycins against Aspergillus flavus FBCC 2467. Structural and genetic information of heinamides may prove useful in future discovery of natural products and drug development.

摘要

拉沙菌素是一类具有协同抗真菌和抗增殖活性的环状脂肽。它们由多种蓝藻属产生,由两组结构上无关的 11 位和 12 位残基大环脂肽组成。在这里,我们通过抗菌生物活性筛选报告了从 Nostoc sp. UHCC 0702 中发现的新的抗真菌拉沙菌素,我们将其命名为海纳米德。我们对 8 种海纳米德结构变体 A1-A3 和 B1-B5 进行了化学结构表征。这些变体包含罕见的非蛋白质氨基酸 3-羟基-4-甲基脯氨酸、4-羟基脯氨酸、3-羟基-d-亮氨酸、脱氢丁氨酸、5-羟基β-氨基辛酸和 O-氨甲酰-高丝氨酸。我们从 Nostoc sp. UHCC 0702 获得了一个 8.6-Mb 的完整基因组序列,并鉴定了 93kb 的海纳米德生物合成基因簇。结构不同的海纳米德 A1-A3 和 B1-B5 变体使用一种不寻常的分支生物合成途径合成。海纳米德生物合成途径还编码几种将非蛋白质氨基酸供应给海纳米德合成酶的酶。通过异源表达,我们表明 (2S,4R)-4-羟基-l-脯氨酸是通过一种新型酶 LxaN 的作用提供的,该酶使 l-脯氨酸羟基化。11 位和 12 位残基的海纳米德具有拉沙菌素对 Aspergillus flavus FBCC 2467 的协同活性。海纳米德的结构和遗传信息可能有助于未来天然产物的发现和药物开发。

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