具有有趣酮基的一系列海洋衍生 14 单元 Resorcylic Acid 内酯的半合成、结构解析和抗褐藻分枝杆菌活性。

IF 4.9 2区 医学 Q1 CHEMISTRY, MEDICINAL Marine Drugs Pub Date : 2024-09-25 DOI:10.3390/md22100431
Jun-Na Yin, Cui-Fang Wang, Xiu-Li Zhang, Ya-Jie Cheng, Yan-Wei Wu, Qun Zhang, Chang-Lun Shao, Mei-Yan Wei, Yu-Cheng Gu
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The <i>R</i>/<i>S</i> configuration of the diastereoisomer at C-13' was further determined through an NOE correlation analysis of CH<sub>3</sub> or CH<sub>2</sub> at the derivative C-13' position and the H-5' and H-6' by means of a 1D NOE experiment. Further comparative <sup>1</sup>H NMR analysis of diastereoisomers showed the difference in the chemical shift (<i>δ</i>) value of the diastereoisomers. The synthetic compounds were screened for their anti-microbial activities in vitro. Compounds <b>15</b>-<b>24</b> and <b>28</b>-<b>35</b> demonstrated promising activity against <i>M. marinum</i>, with MIC<sub>90</sub> values ranging from 70 to 90 μM, closely approaching the MIC<sub>90</sub> of isoniazid. The preliminary structure-activity relationships showed that the ketal groups with aromatic rings at C-5' and C-6' could enhance the inhibition of <i>M. marinum</i>. 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引用次数: 0

摘要

马氏分枝杆菌感染的发病率呈上升趋势,但现有药物治疗周期长,往往需要多种药物联合使用。因此,有必要开发新的、有效的抗马氏分枝杆菌药物。Cochliomycin A 是一种 14 元共轭酸内酯,在 C-5' 和 C-6' 位有一个丙酮基团,具有广泛的抗菌、抗疟和防污活性。为了进一步探究 C-5' 和 C-6' 结构变化对该化合物活性的影响,我们合成了一系列结构与霉素 A 相似,但在 C-5' 和 C-6' 含有缩酮基团的化合物。通过一维 NOE 实验对衍生物 C-13' 位上的 CH3 或 CH2 与 H-5' 和 H-6' 的相关性进行分析,进一步确定了 C-13' 非对映异构体的 R/S 构型。非对映异构体的进一步比较 1H NMR 分析表明,非对映异构体的化学位移(δ)值存在差异。对合成化合物进行了体外抗微生物活性筛选。化合物 15-24 和 28-35 对 M. marinum 表现出了良好的活性,其 MIC90 值在 70 到 90 μM 之间,接近异烟肼的 MIC90 值。初步的结构-活性关系表明,C-5'和 C-6' 位芳香环上的酮基能增强对马林霉素的抑制作用。进一步的研究表明,化合物 23、24、29 和 30 对 M. marinum 有显著的抑制作用,并与异烟肼和利福平有成瘾效应。它的有效特性使其成为未来开发抗马林菌耐药性药物的重要线索。
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Semisynthesis, Structure Elucidation and Anti-Mycobacterium marinum Activity of a Series of Marine-Derived 14-Membered Resorcylic Acid Lactones with Interesting Ketal Groups.

The incidence of Mycobacterium marinum infection is on the rise; however, the existing drug treatment cycle is lengthy and often requires multi-drug combination. Therefore, there is a need to develop new and effective anti-M. marinum drugs. Cochliomycin A, a 14-membered resorcylic acid lactone with an acetonide group at C-5' and C-6', exhibits a wide range of antimicrobial, antimalarial, and antifouling activities. To further explore the effect of this structural change at C-5' and C-6' on this compound's activity, we synthesized a series of compounds with a structure similar to that of cochliomycin A, bearing ketal groups at C-5' and C-6'. The R/S configuration of the diastereoisomer at C-13' was further determined through an NOE correlation analysis of CH3 or CH2 at the derivative C-13' position and the H-5' and H-6' by means of a 1D NOE experiment. Further comparative 1H NMR analysis of diastereoisomers showed the difference in the chemical shift (δ) value of the diastereoisomers. The synthetic compounds were screened for their anti-microbial activities in vitro. Compounds 15-24 and 28-35 demonstrated promising activity against M. marinum, with MIC90 values ranging from 70 to 90 μM, closely approaching the MIC90 of isoniazid. The preliminary structure-activity relationships showed that the ketal groups with aromatic rings at C-5' and C-6' could enhance the inhibition of M. marinum. Further study demonstrated that compounds 23, 24, 29, and 30 had significant inhibitory effects on M. marinum and addictive effects with isoniazid and rifampicin. Its effective properties make it an important clue for future drug development toward combatting M. marinum resistance.

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来源期刊
Marine Drugs
Marine Drugs 医学-医药化学
CiteScore
9.60
自引率
14.80%
发文量
671
审稿时长
1 months
期刊介绍: Marine Drugs (ISSN 1660-3397) publishes reviews, regular research papers and short notes on the research, development and production of drugs from the sea. Our aim is to encourage scientists to publish their experimental and theoretical research in as much detail as possible, particularly synthetic procedures and characterization information for bioactive compounds. There is no restriction on the length of the experimental section.
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