Absolute stereochemistry and anti-inflammatory activity of cycloisobrachycoumarin, brachycromone, cyclobrachycoumarin, and cyclobrachycoumarin 2’-epimer from Gerbera delavayi

IF 1.3 4区生物学 Q4 CHEMISTRY, MEDICINAL

Phytochemistry Letters Pub Date : 2024-04-16 DOI:10.1016/j.phytol.2024.04.011

Yong-xun Yang , Qun Wang , Xiao-nian Li , Hai-yan Huang , Hao Geng

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Abstract

Four isomeric 5-methyl-4-hydroxycoumarin-monoterpene hybrids (MMHs) comprising three known MMHs, cycloisobrachycoumarin (1), brachycromone (2), cyclobrachycoumarin (3), and a new epimer of 3, cyclobrachycoumarin 2’-epimer (4) were isolated from Gerbera delavayi. The absolute configuration of 1–4 was elucidated by utilizing ECD calculations and X-ray diffraction analysis. As a result, the absolute configurations of C-2’ and C-3’ in 1 and 2 were revised to be 2′S, 3′R and 2′R, 3′S respectively. Consequently, the diagnostic negative/positive cotton effect (CE) at around 210–220 nm for the stereochemistry of angular/linear furano-MMHs is discussed and formulated. Moreover, compounds 1–4 were tested for the nitric oxide (NO) inhibitory activity by using lipopolysaccharide (LPS)-induced RAW 264.7 cells in vitro. The results showed that 1–4 significantly inhibited NO production at the concentration of 10.0 μM, indicating that 1–4 possessed potent anti-inflammatory activity.

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来自非洲菊的环异布拉香豆素、布拉香豆酮、环布拉香豆素和环布拉香豆素 2'-epimer 的绝对立体化学和抗炎活性

从非洲菊中分离出四种异构的 5-甲基-4-羟基香豆素-单萜混合物（MMHs），包括三种已知的 MMHs：环异布拉香豆素（1）、布拉香豆酮（2）、环布拉香豆素（3），以及 3 的一种新的表聚体--环布拉香豆素 2'- 表聚体（4）。通过 ECD 计算和 X 射线衍射分析，阐明了 1-4 的绝对构型。结果，1 和 2 中 C-2' 和 C-3' 的绝对构型分别被修正为 2′S, 3′R 和 2′R, 3′S。因此，讨论并提出了角/线性呋喃-MMHs 立体化学的诊断性负/正棉花效应（CE），波长约为 210-220nm。此外，还利用脂多糖（LPS）诱导的 RAW 264.7 细胞对化合物 1-4 的一氧化氮（NO）抑制活性进行了体外测试。结果表明，在 10.0 μM 的浓度下，1-4 能明显抑制一氧化氮的产生，表明 1-4 具有很强的抗炎活性。

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来源期刊

Phytochemistry Letters 生物-生化与分子生物学

CiteScore

3.00

自引率

11.80%

发文量

190

审稿时长

34 days

期刊介绍： Phytochemistry Letters invites rapid communications on all aspects of natural product research including: • Structural elucidation of natural products • Analytical evaluation of herbal medicines • Clinical efficacy, safety and pharmacovigilance of herbal medicines • Natural product biosynthesis • Natural product synthesis and chemical modification • Natural product metabolism • Chemical ecology • Biotechnology • Bioassay-guided isolation • Pharmacognosy • Pharmacology of natural products • Metabolomics • Ethnobotany and traditional usage • Genetics of natural products Manuscripts that detail the isolation of just one new compound are not substantial enough to be sent out of review and are out of scope. Furthermore, where pharmacology has been performed on one new compound to increase the amount of novel data, the pharmacology must be substantial and/or related to the medicinal use of the producing organism.