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Discovery of a Natural Syk Inhibitor from Chinese Medicine through a Docking-Based Virtual Screening and Biological Assay Study

机译:通过基于对接的虚拟筛选和生物学分析研究从中药中发现天然的Syk抑制剂。

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摘要

Spleen tyrosine kinase (Syk) is a critical target protein for treating immunoreceptor signalling-mediated allergies. In this study, a virtual screening of an in-house Chinese medicine database followed by biological assays was carried out to identify novel Syk inhibitors. A molecular docking method was employed to screen for compounds with potential Syk inhibitory activity. Then, an in vitro kinase inhibition assay was performed to verify the Syk inhibitory activity of the virtual screening hits. Subsequently, a β-hexosaminidase release assay was conducted to evaluate the anti-mast cell degranulation activity of the active compounds. Finally, tanshinone I was confirmed as a Syk inhibitor (IC50 = 1.64 μM) and exhibited anti-mast cell degranulation activity in vitro (IC50 = 2.76 μM). Docking studies showed that Pro455, Gln462, Leu377, and Lys458 were key amino acid residues for Syk inhibitory activity. This study demonstrated that tanshinone I is a Syk inhibitor with mast cell degranulation inhibitory activity. Tanshinone I may be a potential lead compound for developing effective and safe Syk-inhibiting drugs.
机译:脾酪氨酸激酶(Syk)是用于治疗免疫受体信号介导的过敏反应的关键靶蛋白。在这项研究中,对内部中药数据库进行了虚拟筛选,然后进行了生物学分析,以鉴定新型Syk抑制剂。使用分子对接方法来筛选具有潜在Syk抑制活性的化合物。然后,进行体外激酶抑制试验以验证虚拟筛选命中的Syk抑制活性。随后,进行β-己糖胺酶释放测定以评估活性化合物的抗肥大细胞脱粒活性。最后,丹参酮I被确认为Syk抑制剂(IC50 = 1.64μM),并在体外表现出抗肥大细胞脱粒活性(IC50 = 2.76μM)。对接研究表明Pro455,Gln462,Leu377和Lys458是抑制Syk的关键氨基酸残基。这项研究证明丹参酮I是具有肥大细胞脱粒抑制活性的Syk抑制剂。丹参酮I可能是开发有效且安全的Syk抑制药物的潜在先导化合物。

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