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Total Synthesis and Biological Evaluation of Apratoxin E and Its C30 Epimer: Configurational Reassignment of the Natural Product.阿普拉毒素E及其C30差向异构体的全合成与生物学评价:天然产物的构型重新确定
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Incorporation of Privileged Structures into Bevirimat Can Improve Activity against Wild-Type and Bevirimat-Resistant HIV-1.将优势结构引入比维莫德可提高其对野生型和比维莫德耐药的HIV-1的活性。
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The evolution of genome mining in microbes - a review.微生物中基因组挖掘的演变——综述。
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Apratoxin Kills Cells by Direct Blockade of the Sec61 Protein Translocation Channel.Apratoxin 通过直接阻断 Sec61 蛋白易位通道杀死细胞。
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Natural Products as Sources of New Drugs from 1981 to 2014.1981年至2014年作为新药来源的天然产物
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antiSMASH 3.0-a comprehensive resource for the genome mining of biosynthetic gene clusters.antiSMASH 3.0——用于生物合成基因簇基因组挖掘的综合资源。
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Directed natural product biosynthesis gene cluster capture and expression in the model bacterium Bacillus subtilis.定向天然产物生物合成基因簇的捕获及其在模式细菌枯草芽孢杆菌中的表达
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Recent advances in natural product discovery.天然产物发现的最新进展。
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一种用于发现天然产物的基质辅助激光解吸电离质谱同位素方法:隐马尔地酰胺,一种来自海洋蓝藻莫雷阿岛原绿球藻的杂合三肽。

A Maldiisotopic Approach to Discover Natural Products: Cryptomaldamide, a Hybrid Tripeptide from the Marine Cyanobacterium Moorea producens.

作者信息

Kinnel Robin B, Esquenazi Eduardo, Leao Tiago, Moss Nathan, Mevers Emily, Pereira Alban R, Monroe Emily A, Korobeynikov Anton, Murray Thomas F, Sherman David, Gerwick Lena, Dorrestein Pieter C, Gerwick William H

机构信息

Department of Chemistry, Hamilton College , Clinton, New York 13323, United States.

Department of Biology, William Paterson University of New Jersey , Wayne, New Jersey 07470, United States.

出版信息

J Nat Prod. 2017 May 26;80(5):1514-1521. doi: 10.1021/acs.jnatprod.7b00019. Epub 2017 Apr 27.

DOI:10.1021/acs.jnatprod.7b00019
PMID:28448144
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5748289/
Abstract

Genome sequencing of microorganisms has revealed a greatly increased capacity for natural products biosynthesis than was previously recognized from compound isolation efforts alone. Hence, new methods are needed for the discovery and description of this hidden secondary metabolite potential. Here we show that provision of heavy nitrogen N-nitrate to marine cyanobacterial cultures followed by single-filament MALDI analysis over a period of days was highly effective in identifying a new natural product with an exceptionally high nitrogen content. The compound, named cryptomaldamide, was subsequently isolated using MS to guide the purification process, and its structure determined by 2D NMR and other spectroscopic and chromatographic methods. Bioinformatic analysis of the draft genome sequence identified a 28.7 kB gene cluster that putatively encodes for cryptomaldamide biosynthesis. Notably, an amidinotransferase is proposed to initiate the biosynthetic process by transferring an amidino group from arginine to serine to produce the first residue to be incorporated by the hybrid NRPS-PKS pathway. The maldiisotopic approach presented here is thus demonstrated to provide an orthogonal method by which to discover novel chemical diversity from Nature.

摘要

微生物的基因组测序显示,其天然产物生物合成能力比之前仅通过化合物分离工作所认识到的要大大增强。因此,需要新的方法来发现和描述这种隐藏的次生代谢产物潜力。在此,我们表明,向海洋蓝藻培养物中提供重氮N-硝酸盐,随后在数天内进行单丝基质辅助激光解吸电离(MALDI)分析,对于鉴定一种氮含量异常高的新天然产物非常有效。该化合物名为隐马尔地酰胺,随后利用质谱引导纯化过程将其分离,并通过二维核磁共振(2D NMR)以及其他光谱和色谱方法确定其结构。对基因组草图序列进行的生物信息学分析鉴定出一个28.7 kB的基因簇,推测其编码隐马尔地酰胺的生物合成。值得注意的是,有人提出一种脒基转移酶通过将脒基从精氨酸转移到丝氨酸来启动生物合成过程,从而产生第一个由NRPS-PKS杂交途径掺入的残基。因此,本文介绍的MALDI同位素方法被证明是一种从自然界发现新化学多样性的正交方法。