摘要
目的利用假病毒技术,研究来源于马尾树树皮的化合物蜡果杨梅酸B抑制HIV-1进入的活性及作用机制。方法利用pHXB2和pVSV-G两个病毒包膜蛋白质粒,与pNL4-3.Luc.R-E-共转染,构建HIV-1Env假病毒和VSV-G假病毒,检测化合物抑制假病毒感染的活性。采用针对包膜蛋白亚基gp41的ELISA方法,结合分子对接,研究活性化合物抗HIV-1的作用机制。结果从马尾树树皮中来源的2个三萜类单体化合物蜡果杨梅酸B(myriceric acid B)和蜡果杨梅酸C(myriceric acid C)中,仅蜡果杨梅酸B能特异性地抑制HIV-1 Env假病毒感染,其半数抑制浓度(IC50)值为(8.3±0.2)mg·L-1。此外,蜡果杨梅酸B在C-28位羧基的酯化产物蜡果杨梅酸B甲酯(myriceric acid B methyl ester)没有抑制HIV-1进入的活性。蜡果杨梅酸B的进入抑制活性与其抑制gp41六螺旋束结构形成的机制有关。分子对接表明,蜡果杨梅酸B能靶向gp41上N-螺旋三聚体的靶穴位置。结论蜡果杨梅酸B是作用于gp41的HIV-1进入抑制剂,其分子结构中C-28位的羧基及C-3位羟基与抑制活性密切相关。蜡果杨梅酸B可作为先导化合物来研发新的HIV进入抑制剂类抗艾滋病药物。
Aim To investigate the HIV-1 entry inhibitory activities of myriceric acid B and C isolated from Rhoiptelea chiliantha Diels et Hand-Mazz and their mechanism of action.Method The plasmids encodingenvelope proteins of HIV-1 (pHXB2) and VSV (pVSV-G) were cotransfected 293T cells with pNL4-3.Luc.R-E- to produce HIV-1 Env pseudovirus and VSV-G pseudovirus,respectively,which were used for testing the antiviral activities of these compounds.ELISA and molecular docking were used to study the mechanism of action of the active compounds.Results Myriceric acid B could significantly inhibit the infection of HIV-1 Env pseudovirus with an IC50 of(8.3±0.2)mg·L^-1.The carbonoxyl group at C-28 position and the hydroxyl group at the C-3 position of myriceric acid B are important for its anti-HIV-1 activity.Like other HIV-1 entry inhibitors targeting gp41 (eg,ADS-J1 and NB-64), myriceric acid B could also block the gp41 six-helix bundle formation.Molecular docking analysis suggests that myriceric acid B may bind to the hydrophobic cavity of the gp41 N-trimeric coiled coil.Conclusion Myriceric acid B is a potent HIV-1 entry inhibitor targeting gp41 and can serve as a lead compound for developing novel anti-HIV-1 drug.
出处
《中国药理学通报》
CAS
CSCD
北大核心
2010年第4期447-452,共6页
Chinese Pharmacological Bulletin
基金
国家自然科学基金资助项目(No30729001
U0832001)
