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真菌肽生物碱生物合成中的复杂性生成:黄曲霉菌 Af12070 黄素酶氧化呋喹唑啉 A 生成七环半缩醛呋喹唑啉 C。

Complexity generation in fungal peptidyl alkaloid biosynthesis: oxidation of fumiquinazoline A to the heptacyclic hemiaminal fumiquinazoline C by the flavoenzyme Af12070 from Aspergillus fumigatus.

机构信息

Department of Biological Chemistry & Molecular Pharmacology, Harvard Medical School, Boston, Massachusetts 02115, United States.

出版信息

Biochemistry. 2011 Oct 11;50(40):8756-69. doi: 10.1021/bi201302w. Epub 2011 Sep 19.

Abstract

The human pathogen Aspergillus fumigatus makes a series of fumiquinazoline (FQ) peptidyl alkaloids of increasing scaffold complexity using L-Trp, 2 equiv of L-Ala, and the non-proteinogenic amino acid anthranilate as building blocks. The FQ gene cluster encodes two non-ribosomal peptide synthetases (NRPS) and two flavoproteins. The trimodular NRPS Af12080 assembles FQF (the first level of complexity) while the next two enzymes, Af12060 and Af12050, act in tandem in an oxidative annulation sequence to couple alanine to the indole side chain of FQF to yield the imidazolindolone-containing FQA. In this study we show that the fourth enzyme, the monocovalent flavoprotein Af12070, introduces a third layer of scaffold complexity by converting FQA to the spirohemiaminal FQC, presumably by catalyzing the formation of a transient imine within the pyrazinone ring (and therefore acting in an unprecedented manner as an FAD-dependent amide oxidase). FQC subsequently converts nonenzymatically to the known cyclic aminal FQD. We also investigated the effect of substrate structure on Af12070 activity and subsequent cyclization with a variety of FQA analogues, including an FQA diastereomer (2'-epi-FQA), which is an intermediate in the fungal biosynthesis of the tremorgenic tryptoquialanine. 2'-epi-FQA is processed by Af12070 to epi-FQD, not epi-FQC, illustrating that the delicate balance in product cyclization regiochemistry can be perturbed by a remote stereochemical center.

摘要

人类病原体烟曲霉(Aspergillus fumigatus)使用 L-Trp、2 当量的 L-Ala 和非蛋白氨基酸邻氨基苯甲酸作为构建块,生成一系列结构复杂度不断增加的 fumiquinazoline (FQ) 肽基生物碱。FQ 基因簇编码两个非核糖体肽合酶 (NRPS) 和两个黄素蛋白。三模块 NRPS Af12080 组装 FQF(第一级复杂度),而接下来的两个酶 Af12060 和 Af12050 在氧化环合序列中串联作用,将丙氨酸偶联到 FQF 的吲哚侧链上,生成含有咪唑并吲哚酮的 FQA。在这项研究中,我们表明第四个酶,单价黄素蛋白 Af12070,通过将 FQA 转化为螺环半亚胺 FQC,引入了第三层结构复杂性,推测是通过在吡嗪酮环内形成瞬态亚胺(因此以前所未有的方式作为 FAD 依赖的酰胺氧化酶发挥作用)。FQC 随后非酶促转化为已知的环状亚胺 FQD。我们还研究了底物结构对 Af12070 活性的影响以及与各种 FQA 类似物的后续环化作用,包括 FQA 差向异构体(2'-epi-FQA),它是真菌生物合成震颤原性 tryptoquialanine 的中间产物。2'-epi-FQA 被 Af12070 加工成 epi-FQD,而不是 epi-FQC,这表明产物环化区域化学的微妙平衡可以被远程立体化学中心干扰。

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