PPARα/γ-靶向甘草地上部分的阿莫鲁丁植物大麻素。

IF 3.3 2区 生物学 Q2 CHEMISTRY, MEDICINAL
Elena Serino, Fabio Arturo Iannotti, Hekmat B. Al-Hmadi, Diego Caprioglio, Claudia Moriello, Francesca Masi, Saoussen Hammami, Giovanni Appendino, Rosa Maria Vitale* and Orazio Taglialatela-Scafati*, 
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引用次数: 0

摘要

LC-MS/MS引导下对甘草地上部分的分析提供了新的苯乙基(阿摩尔)和烷基(大麻)型植物大麻素(分别为6种和4种化合物)。通过分离六个已知成员和合成在芳烷基部分修饰的类似物,补充了新的无定形蛋白的结构多样性。测定由此获得的所有化合物对PPARα和PPARγ核受体的激动剂活性。阿莫鲁丁A(1)对PPARγ表现出最高的激动剂活性,阿莫鲁丁H(7)选择性靶向PPARα,而阿莫鲁丁E(4)表现为双重激动剂,阿莫鲁丁A(11)的戊基类似物无活性。十碳氧基阿摩尔frutin A(2)具有细胞毒性,将其苯乙基部分修饰为苯乙烯基或苯乙炔基保留了这一特性,这表明这些化合物存在另一种生物学情况。通过分子对接和分子动力学模拟相结合的方法,获得了阿摩尔凝集素对PPARα和PPARγ的假定结合模式,为这类化合物的构效关系提供了见解。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

PPARα/γ-Targeting Amorfrutin Phytocannabinoids from Aerial Parts of Glycyrrhiza foetida

PPARα/γ-Targeting Amorfrutin Phytocannabinoids from Aerial Parts of Glycyrrhiza foetida

An LC-MS/MS-guided analysis of the aerial parts of Glycyrrhiza foetida afforded new phenethyl (amorfrutin)- and alkyl (cannabis)-type phytocannabinoids (six and four compounds, respectively). The structural diversity of the new amorfrutins was complemented by the isolation of six known members and the synthesis of analogues modified on the aralkyl moiety. All of the compounds so obtained were assayed for agonist activity on PPARα and PPARγ nuclear receptors. Amorfrutin A (1) showed the highest agonist activity on PPARγ, amorfrutin H (7) selectively targeted PPARα, and amorfrutin E (4) behaved as a dual agonist, with the pentyl analogue of amorfrutin A (11) being inactive. Decarboxyamorfrutin A (2) was cytotoxic, and modifying its phenethyl moiety to a styryl or a phenylethynyl group retained this trait, suggesting an alternative biological scenario for these compounds. The putative binding modes of amorfrutins toward PPARα and PPARγ were obtained by a combined approach of molecular docking and molecular dynamics simulations, which provided insights on the structure–activity relationships of this class of compounds.

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来源期刊
CiteScore
9.10
自引率
5.90%
发文量
294
审稿时长
2.3 months
期刊介绍: The Journal of Natural Products invites and publishes papers that make substantial and scholarly contributions to the area of natural products research. Contributions may relate to the chemistry and/or biochemistry of naturally occurring compounds or the biology of living systems from which they are obtained. Specifically, there may be articles that describe secondary metabolites of microorganisms, including antibiotics and mycotoxins; physiologically active compounds from terrestrial and marine plants and animals; biochemical studies, including biosynthesis and microbiological transformations; fermentation and plant tissue culture; the isolation, structure elucidation, and chemical synthesis of novel compounds from nature; and the pharmacology of compounds of natural origin. When new compounds are reported, manuscripts describing their biological activity are much preferred. Specifically, there may be articles that describe secondary metabolites of microorganisms, including antibiotics and mycotoxins; physiologically active compounds from terrestrial and marine plants and animals; biochemical studies, including biosynthesis and microbiological transformations; fermentation and plant tissue culture; the isolation, structure elucidation, and chemical synthesis of novel compounds from nature; and the pharmacology of compounds of natural origin.
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