The orchestrated feature of Cornus kousa fruit and gut microbiota against obesity via integrated pharmacology

IF 7.4 Q1 FOOD SCIENCE & TECHNOLOGY
Food frontiers Pub Date : 2024-06-18 DOI:10.1002/fft2.435
Ki-Kwang Oh, Sang-Jun Yoon, Sang Youn Lee, Satya Priya Sharma, Sung-Min Won, Jin-Ju Jeong, Dong Joon Kim, Ki-Tae Suk
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Abstract

Cornus kousa fruit (CKF) has been utilized as anti-obesity supplementation in East Asia, including Korea, and gut microbiota (GM) might have synergistic effects on obesity (OB) via its interplay. We aimed to decode molecule(s), mechanism(s), and target(s) on interplay between CKF and GM via network pharmacology analysis. The final targets were analyzed by protein–protein interaction (PPI) networks and a bubble plot. The GM interacted with significant targets identified by the gutMGene database. The relationships among CKF or GM, signaling pathways, targets, and molecules (CGSTM) were plotted by R package. Finally, molecular docking assay and density functional theory (DFT) were performed to validate its affinity. The final targets (22) were selected on OB-responded targets, indicating that interleukin-6 (IL6) was the most crucial protein-coding target on PPI networks. A bubble plot and CGSTM networks suggested that the advanced glycation end-receptor for advanced glycation end products signaling pathway in diabetic complications is inhibited by CKF and peroxisome proliferator–activated receptor (PPAR) signaling pathway is activated by GM. As the most stable conformers, IL6-equol complex was attributed to GM, and PPAR alpha-linoleic acid, PPAR delta-stearic acid, and fatty acid–binding protein 4-dimethyl 2,3-bis(1,3-dimethylindol-2-yl) fumarate complex were attributed to CKF. Noticeably, stearic acid was removed by DFT analysis; all other three molecules were proposed as good electron donators with the higher electronegativity compared with a standard drug (Orlistat). This study shows that integrated pharmacological analysis can enable to decode the unknown relationships between CKF and GM. Overall, this study reveals that the combination of CKF and favorable GM might exert dual therapeutic effects on OB.

Abstract Image

山茱萸果实与肠道微生物群通过综合药理学协同作用防治肥胖症
在包括韩国在内的东亚地区,山茱萸果(CKF)已被用作抗肥胖补充剂,而肠道微生物群(GM)可能会通过其相互作用对肥胖(OB)产生协同效应。我们的目的是通过网络药理学分析,解读 CKF 和 GM 之间相互作用的分子、机制和靶点。我们通过蛋白质-蛋白质相互作用(PPI)网络和气泡图分析了最终目标。基因改造药物与 gutMGene 数据库确定的重要靶点发生了相互作用。用 R 软件包绘制了 CKF 或 GM、信号通路、靶点和分子(CGSTM)之间的关系图。最后,通过分子对接试验和密度泛函理论(DFT)验证其亲和力。最终的靶标(22个)是在OB响应靶标的基础上筛选出来的,表明白细胞介素-6(IL6)是PPI网络中最关键的蛋白编码靶标。气泡图和 CGSTM 网络表明,糖尿病并发症中的高级糖化终末受体信号通路受到 CKF 的抑制,而过氧化物酶体增殖激活受体(PPAR)信号通路则被 GM 激活。作为最稳定的构象,IL6-喹啉复合物归因于 GM,而 PPAR alpha-亚油酸、PPAR delta-硬脂酸和脂肪酸结合蛋白 4-二甲基 2,3-双(1,3-二甲基吲哚-2-基)富马酸复合物归因于 CKF。值得注意的是,通过 DFT 分析,硬脂酸被删除;与标准药物(奥利司他)相比,其他三种分子的电负性更高,因此被认为是良好的电子供体。这项研究表明,综合药理学分析能够破解 CKF 和 GM 之间的未知关系。总之,本研究揭示了 CKF 和有利的 GM 的组合可能对 OB 发挥双重治疗作用。
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来源期刊
CiteScore
10.50
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0.00%
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审稿时长
10 weeks
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