摘要
利用分子对接方法,探究H21对分泌炎症因子的关键蛋白的影响.从引起炎症的经典通路中选取关键靶蛋白,通过Glide分子对接,将H21和原配体、靶蛋白对接.通过二者对接得到分值,筛选与H21结合较好的靶蛋白及关键氨基酸,并分析其二者的相互作用.结果显示:H21与Toll-like通路中关键蛋白IRAK1蛋白结合较好,Glide-gscore为-9.873,优于原配体,H21与IRAK1结合的关键氨基酸为Ile218;理论数据表明:抗炎药物H21可能作用于IRAK1蛋白,通过影响IRAK1蛋白的表达,从而发挥抗炎作用,为揭示H21的抗炎机制和作用靶点提供了理论依据.
The molecular docking method was used to explore the impact of H21 on key proteins secreting inflammatory factors.Key target proteins were selected from the classic pathways that cause inflammation and H21 and the original ligand with the target protein were docked through Glide molecular docking.The target proteins and key amino acids that were well bound to H21 were screened,and the interaction between them was analyzed.The results showed that H21 bound well to the key protein IRAK1 protein in the Toll-like pathway,and the Glide-gscore is-9.873,better than that of the original ligand.The key amino acids for H21 binding to IRAK1 is Ile218.Theoretical data indicated that the anti-inflammatory drug H21 may act on IRAK1 protein,and by affecting the expression of IRAK1 protein,will exert anti-inflammatory effect.That may provide a theoretical basis for the anti-inflammatory mechanism of H21 and its target of action.
作者
宋瑗瑗
曹洪玉
未志俞
王倩
蒋革
SONG Yuanyuan;CAO Hongyu;WEI Zhiyu;WANG Qian;JIANG Ge(School of Life Science and Technology, Dalian University, Dalian 116622, China;School of Medicine, Dalian University, Dalian 116622, China)
出处
《华南师范大学学报(自然科学版)》
CAS
北大核心
2021年第2期59-64,共6页
Journal of South China Normal University(Natural Science Edition)
基金
国家自然科学基金项目(21601025)
大连市高层次创新人才项目(2017RQ156)。
关键词
熊果酸衍生物
分子对接
分子模拟筛选
炎症因子
IRAK1
ursolic acid derivative
molecular docking
molecular simulation screening
inflammatory factor
IRAK1
