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首页> 外文期刊>E3S Web of Conferences >A Network Pharmacology Approach to Investigate the Underlying Mechanisms of Alpinia Katsumadai Hayata on Acne Vulgaris
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A Network Pharmacology Approach to Investigate the Underlying Mechanisms of Alpinia Katsumadai Hayata on Acne Vulgaris

机译:一种网络药理学方法,探讨Alpinia Katsumadai Hayata对寻常痤疮的潜在机制

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The Alpinia katsumadai Hayata Doukou, DK, is a traditional Chinese medicine that has shown superior anti-inflammatory property, which is widely used in the food and commodity industry. A network pharmacology analysis was performed to identify the potential anti-acne compounds, hub therapeutic targets, and the key pathways via TCMSP, BATMAN, CTD, PDB and PubChem databases. Finally, the “compoundtarget- pathway” network was constructed. The study found total 7 active compounds, including quercetin, (2R)-5,7-dihydroxy-2-phenylchroman-4-one, dehydrodiisoeugenol, (2R)-7-hydroxy-5-methoxy-2- phenylchroman-4-one, Pinocembrin, and 1,7-diphenyl-5-hydroxy-6-hepten-3-one alpinolide peroxide. In addition, 30 therapeutic targets, and 4 hub therapeutic targets of the DK were identified. The biological processes were primarily related to inflammatory response, response to oxidative stress, regulation of insulin secretion, etc. Which was significantly associated with ten pathways including the PI3K-Akt signaling pathways, VEGF signaling pathways, etc. Furtherly, the 4 hub targets AKT1, F2, AR, and PTGS2 with higher connectivity in PPI network were verificated though molecular docking, which once again proved that these targets are potential targets of their corresponding chemical molecules. Therefore, DK might have a synergistic effect on the anti-inflammatory effects via the various active compositions, targets and signaling pathways.
机译:DK的Alpinia Katsumadai Hayata Douata Doutkou是一种卓越的抗炎性能,广泛用于食品和商品行业。进行网络药理学分析以通过TCMSP,蝙蝠侠,CTD,PDB和Pubchem数据库鉴定潜在的抗痤疮化合物,轮毂治疗靶标和关键途径。最后,构建了“复合物 - 途径”网络。该研究发现总共7种活性化合物,包括槲皮素,(2R)-5,7-二羟基-2-苯基核醇-4-一,脱氢原因-2-一,(2R)-7-羟基-5-甲氧基-2-苯基卷,Pinocembrin和1,7-二苯基-5-羟基-6-庚烯-3-一羟氢化物过氧化物。另外,鉴定了30个治疗靶标和4个DK的4轮疗法靶标。生物方法主要与炎症反应,对氧化应激的反应,胰岛素分泌调节等有关,其与包括PI3K-AKT信号传导途径,VEGF信号传导途径等的十种途径显着相关的等,4个集线器目标AKT1尽管分子对接,但再次证明这些靶标是它们相应的化学分子的潜在靶标的PPI网络中具有较高连接的PPI网络和PTGS2。因此,DK可能通过各种活性组合物,靶标和信号通路对抗炎作用具有协同作用。

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