Resveratrol analogues and metabolites selectively inhibit human and rat 11β-hydroxysteroid dehydrogenase 1 as the therapeutic drugs: structure-activity relationship and molecular dynamics analysis.

IF 2.3 3区 环境科学与生态学 Q3 CHEMISTRY, MULTIDISCIPLINARY
C Hu, Y Zhai, H Lin, H Lu, J Zheng, C Wen, X Li, R S Ge, Y Liu, Q Zhu
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引用次数: 0

Abstract

Resveratrol is converted to various metabolites by gut microbiota. Human and rat liver 11β-hydroxysteroid dehydrogenase 1 (11β-HSD1) are critical for glucocorticoid activation, while 11β-HSD2 in the kidney does the opposite reaction. It is still uncertain whether resveratrol and its analogues selectively inhibit 11β-HSD1. In this study, the inhibitory strength, mode of action, structure-activity relationship (SAR), and docking analysis of resveratrol analogues on human, rat, and mouse 11β-HSD1 and 11β-HSD2 were performed. The inhibitory strength of these chemicals on human 11β-HSD1 was dihydropinosylvin (6.91 μM) > lunularin (45.44 μM) > pinostilbene (46.82 μM) > resveratrol (171.1 μM) > pinosylvin (193.8 μM) > others. The inhibitory strength of inhibiting rat 11β-HSD1 was pinostilbene (9.67 μM) > lunularin (17.39 μM) > dihydropinosylvin (19.83 μM) > dihydroresveratrol (23.07 μM) > dihydroxystilbene (27.84 μM) > others and dihydropinosylvin (85.09 μM) and pinostilbene (>100 μM) inhibited mouse 11β-HSD1. All chemicals did not inhibit human, rat, and mouse 11β-HSD2. It was found that dihydropinosylvin, lunularin, and pinostilbene were competitive inhibitors of human 11β-HSD1 and that pinostilbene, lunularin, dihydropinosylvin, dihydropinosylvin and dihydroxystilbene were mixed inhibitors of rat 11β-HSD1. Docking analysis showed that they bind to the steroid-binding site of human and rat 11β-HSD1. In conclusion, resveratrol and its analogues can selectively inhibit human and rat 11β-HSD1, and mouse 11β-HSD1 is insensitive to the inhibition of resveratrol analogues.

白藜芦醇类似物和代谢物选择性抑制人和大鼠 11β- 羟基类固醇脱氢酶 1 的治疗药物:结构-活性关系和分子动力学分析。
白藜芦醇会被肠道微生物群转化为各种代谢物。人和大鼠肝脏中的 11β-羟类固醇脱氢酶 1(11β-HSD1)对糖皮质激素的激活至关重要,而肾脏中的 11β-HSD2 则起相反的作用。本研究对白藜芦醇及其类似物对人、大鼠和小鼠 11β-HSD1 和 11β-HSD2 的抑制强度、作用模式、结构-活性关系(SAR)和对接分析进行了研究。这些化学物质对人类 11β-HSD1 的抑制强度依次为:二氢吡咯乙烯(6.91 μM)>月桂苷(45.44 μM)>松芪(46.82 μM)>白藜芦醇(171.1 μM)>吡咯乙烯(193.8 μM)>其他。对大鼠 11β-HSD1 的抑制强度为:松芪(9.67 μM)>月桂苷(17.39 μM)>二氢白藜芦醇(19.83 μM)>二氢白藜芦醇(23.07 μM)>二羟基白藜芦醇(27.84 μM)>其他;二氢白藜芦醇(85.09 μM)和松芪(>100 μM)对小鼠 11β-HSD1 的抑制强度为:松芪(9.67 μM)>月桂苷(17.39 μM)>二氢白藜芦醇(19.83 μM)>二羟基白藜芦醇(23.07 μM)>二羟基白藜芦醇(27.84 μM)>其他。所有化学物质对人、大鼠和小鼠的 11β-HSD2 都没有抑制作用。研究发现,二氢赤松素、月桂苷和松芪是人 11β-HSD1 的竞争性抑制剂,松芪、月桂苷、二氢赤松素、二氢赤松素和二羟基芪是大鼠 11β-HSD1 的混合抑制剂。总之,白藜芦醇及其类似物能选择性地抑制人和大鼠的 11β-HSD1,而小鼠的 11β-HSD1 对白藜芦醇类似物的抑制作用不敏感。
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来源期刊
CiteScore
5.20
自引率
20.00%
发文量
78
审稿时长
>24 weeks
期刊介绍: SAR and QSAR in Environmental Research is an international journal welcoming papers on the fundamental and practical aspects of the structure-activity and structure-property relationships in the fields of environmental science, agrochemistry, toxicology, pharmacology and applied chemistry. A unique aspect of the journal is the focus on emerging techniques for the building of SAR and QSAR models in these widely varying fields. The scope of the journal includes, but is not limited to, the topics of topological and physicochemical descriptors, mathematical, statistical and graphical methods for data analysis, computer methods and programs, original applications and comparative studies. In addition to primary scientific papers, the journal contains reviews of books and software and news of conferences. Special issues on topics of current and widespread interest to the SAR and QSAR community will be published from time to time.
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