共查询到19条相似文献,搜索用时 109 毫秒
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金丝桃素分子结构及其与HIV病毒蛋白酶作用的分子动力学研究 总被引:2,自引:0,他引:2
采用用计算化学方法研究金丝桃素分子结构特征, 并用分子动力学方法研究其与HIV蛋白酶的相互作用, 探讨其可能的抗HIV病毒作用机理. 结果表明, 金丝桃素分子结构具有刚性特征, 与HIV蛋白酶在酶的催化活性位点与ASP-A25 and ASP-B25以氢键作用相结合. 相似文献
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贯叶连翘中金丝桃素提取工艺的研究 总被引:17,自引:0,他引:17
贯叶连翘为藤黄科金丝桃属(HypericumL.)植物贯叶连翘(HypericumperformatumL.)的全草,它主要被用于抗菌消炎、收敛止血、治吐血、外伤出血、肿毒及止痛等症[1]。近年来国外的研究发现,金丝桃素是贯叶连翘中的最主要有效成分。... 相似文献
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在模拟生理条件下,采用荧光、共振散射、圆二色谱(CD)等光谱法和原子力显微镜及分子对接技术,研究了金丝桃苷与人血清白蛋白(HSA)的相互作用。应用分子对接技术预测金丝桃苷结合在HSA的SiteⅠ位,预测结果与位点探针竞争实验结果吻合。原子力显微镜(AFM)图像和共振散射光谱表明,与金丝桃苷结合后HSA的分子直径变大,产生相互聚集。金丝桃苷对HSA内源荧光的猝灭机制属于形成基态复合物所引起的静态猝灭。测得的热力学参数表明,金丝桃苷与HSA作用主要由疏水作用和氢键驱动。根据Frster非辐射能量转移理论求得两者间的结合距离为3.52nm。CD谱显示金丝桃苷诱导HSA的二级结构产生稍许的变化。 相似文献
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利用阳离子聚噻吩衍生物与单链DNA和杂合体DNA/RNA通过静电相结合时所产生的紫外吸收变化,建立了一种检测HIV逆转录酶(RT-HIV)的RNase H活性的方法。阳离子聚噻吩衍生物的紫外吸收最大波长位于短波385nm,与单链DNA结合会使聚噻吩衍生物的紫外吸收最大波长红移至525nm;而与杂合体DNA/RNA结合时对其紫外吸收最大波长几乎没有影响,当利用RT-HIV的核糖核酸酶RNase H活性水解掉杂合体中的RNA时,杂合体溶液又会使聚噻吩衍生物的紫外吸收最大波长发生红移。结果表明,紫外吸收最大波长变化明显,甚至直观用肉眼就可以观察到杂合体水解前后溶液颜色的变化。同时还测定了不同时间下RNase H酶水解杂合体中RNA的吸光度变化曲线,计算出了RNase H酶水解的动力学常数和最大初速度。 相似文献
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颗粒型甲烷单加氧酶(Particulate methane monooxygenase, PMMO)是一个与细胞膜结合的金属酶, 能将烷烃生物催化为醇. 研究PMMO与烷烃的结合模式及催化机制将有利于设计合成一个新的模拟酶, 进而有效地利用烷烃作为新能源. 用分子对接方法获得了PMMO单体与一系列烷烃的结合模式, 并对PMMO单体和PMMO-戊烷复合物进行了6 ns的分子动力学模拟, 最后对复合物进行了构象成簇及结合能分析. 结果表明, 戊烷结合到靠近Zn2+的疏水口袋中, 该口袋由pmoA亚基的M45~W60和R190~T193以及pmoC亚基的Q161三个片段组成. 动力学结果表明, 与PMMO单体比, PMMO-戊烷复合物保持着相近的运动模式, 但幅度更明显, 另外, 戊烷在疏水口袋中的大幅度运动对于PMMO发挥催化作用是必须的. 结合能计算揭示疏水相互作用是戊烷与PMMO稳定识别的主要驱动力, 所有模拟结果与实验数据吻合较好. 相似文献
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金丝桃苷与牛血清白蛋白相互作用的研究 总被引:1,自引:0,他引:1
采用荧光共振能量转移法研究了金丝桃苷与牛血清白蛋白的相互作用.金丝桃苷对牛血清白蛋白(BSA)的荧光猝灭类型是静态猝灭,25℃时的结合位点数为0.5451.并依据F(o)ster非辐射能量转移理论,研究了给体(牛血清白蛋白)--受体(金丝桃苷)间的结合距离R.和能量转移效率E分别为2.04nm和0.66.同时,采用同步... 相似文献
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基于“底物包膜”假说筛选新型HIV-1蛋白酶抑制剂 总被引:1,自引:0,他引:1
基于“底物包膜”假说, 以现有HIV-1蛋白酶抑制剂Darunavir为模板构建药效团模型并对中药化学数据库进行搜索; 采用分子对接方法进一步考察化合物与HIV-1蛋白酶结合情况及其与“底物包膜”符合程度, 优先选出两个化合物Annomonicin和去乙酰蟾蜍它灵; 应用分子动力学方法对这两个化合物进行动力学模拟, 观察它们与蛋白酶结合的复合物在动力学过程中的稳定性并计算其结合自由能, 综合评价筛选结果, 最终确定化合物Annomonicin具有更潜在的深入研究价值. 相似文献
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Human immunodeficiency virus type 1 (HIV-1) integrase (IN) is an essential enzyme in the lifecycle of this virus and also an important target for the study of anti-HIV drugs. The binding mode of the wild type IN core domain and its G140S mutant with L-Chicoric acid (LCA) inhibitor were investigated by using multiple conformation molecular docking and molecular dynamics (MD) simulation. Based on the binding modes, the drug resistance mechanism was explored for the G140S mutant of IN with LCA. The results indicate that the binding site of the G140S mutant of IN core domain with LCA is different from that of the core domain of the wild type IN, which leads to the partial loss of inhibition potency of LCA. The flexibility of the IN functional loop region and the interactions between Mg2 ion and the three key residues (i.e., D64, D116, E152) stimulate the biological operation of IN. The drug resistance also lies in several other important effects, such as the repulsion between LCA and E152 in the G140S mutant core domain, the weakening of K159 binding with LCA and Y143 pointing to the pocket of the G140S mutant. All of the above simulation results agree well with experimental data, which provide us with some helpful information for designing the drug of anti-HIV based on the structure of IN. 相似文献
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用分子对接程序(Autodock)将含有一个Mg2+的HIV-1整合酶核心区(以下简称IN-A)与抑制剂小分子金精三羧酸(简称Aurin)进行对接,预测其未知的复合物结构,然后用分子动力学(MD)方法对IN-A与Aurin的对接结果进行了950 ps的模拟.MD模拟结果发现,IN-A与Aurin形成了两个稳定的氢键,Mg2+也与Aurin上的氧原子形成了稳定的配键,IN-A与Aurin之间的静电相互作用能和范德华相互作用能的平均值分别为-205.8和-162.7 kJ/mol.根据MD模拟得到的IN-A与Aurin相互作用后的构象变化信息,我们对对接复合物结构进行了修正,给出了更加合理和稳定的复合物预测结构.本工作得到的HIV-1整合酶与抑制剂Aurin的结合模式信息将有助于设计和改造出效果更好的抗HIV-1整合酶的先导化合物. 相似文献
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Integrase(IN) plays an essential role in the process of HIV-1 replication.IN inhibitors of diketo acid derivatives(DKAs) were analysed by the Comparative Molecular Field Analysis(CoMFA) and Comparative Molecular Similarity Induces Analysis(CoMSIA) methods.A set of 42 compounds were randomly selected as the training set(35) and test set(7).Firstly,a good pharmacophore(goodness of hit=0.787) was obtained and used to align ligands.Then,predictive models were constructed with the CoMFA and CoMSIA methods based on the pharmacophore alignment.As a result,the CoMS1A method yielded the best model with an r2 of 0.955 and a q2 of 0.665,which can predict the activities of the tested DKAs very well(r2=0.559).Finally,DKAs were docked into IN,and the predicit modes were superimposed on the contour maps obtained from the best CoMSIA model.The superimposed maps gave a visualized and meaningful insight into the inhibitory behaviors,providing significantly useful information for the rational drug design of anti-IN agents. 相似文献
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Arthit Makarasen Suwicha Patnin Pongsit Vijitphan Nanthawan Reukngam Panita Khlaychan Mayuso Kuno Pakamas Intachote Busakorn Saimanee Suchada Sengsai Supanna Techasakul 《Molecules (Basel, Switzerland)》2022,27(2)
New target molecules, namely, 2-phenylamino-4-phenoxyquinoline derivatives, were designed using a molecular hybridization approach, which was accomplished by fusing the pharmacophore structures of three currently available drugs: nevirapine, efavirenz, and rilpivirine. The discovery of disubstituted quinoline indicated that the pyridinylamino substituent at the 2-position of quinoline plays an important role in its inhibitory activity against HIV-1 RT. The highly potent HIV-1 RT inhibitors, namely, 4-(2′,6′-dimethyl-4′-formylphenoxy)-2-(5″-cyanopyridin-2″ylamino)quinoline (6b) and 4-(2′,6′-dimethyl-4′-cyanophenoxy)-2-(5″-cyanopyridin-2″ylamino)quinoline (6d) exhibited half-maximal inhibitory concentrations (IC50) of 1.93 and 1.22 µM, respectively, which are similar to that of nevirapine (IC50 = 1.05 µM). The molecular docking results for these two compounds showed that both compounds interacted with Lys101, His235, and Pro236 residues through hydrogen bonding and interacted with Tyr188, Trp229, and Tyr318 residues through π–π stacking in HIV-1 RT. Interestingly, 6b was highly cytotoxic against MOLT-3 (acute lymphoblastic leukemia), HeLA (cervical carcinoma), and HL-60 (promyeloblast) cells with IC50 values of 12.7 ± 1.1, 25.7 ± 0.8, and 20.5 ± 2.1 µM, respectively. However, 6b and 6d had very low and no cytotoxicity, respectively, to-ward normal embryonic lung (MRC-5) cells. Therefore, the synthesis and biological evaluation of 2-phenylamino-4-phenoxyquinoline derivatives can serve as an excellent basis for the development of highly effective anti-HIV-1 and anticancer agents in the near future. 相似文献
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用分子对接方法研究HIV-1整合酶与病毒DNA的结合模式 总被引:2,自引:0,他引:2
用分子对接方法研究了HIV-1整合酶(Integrase, IN)二聚体与3’ 端加工(3’ Processing, 3’-P)前的8 bp及27 bp病毒DNA的相互作用, 并获得IN与27 bp病毒DNA的特异性结合模式. 模拟结果表明, IN有特异性DNA结合区和非特异性DNA结合区; IN二聚体B链的K14, R20, K156, K159, K160, K186, K188, R199和A链的K219, W243, K244, R262, R263是IN结合病毒DNA的关键残基; 并从结构上解释了能使IN发挥活性的病毒DNA的最小长度是15 bp. 通过分析结合能发现, IN与DNA稳定结合的主要因素是非极性相互作用, 而关键残基与病毒DNA相互识别主要依赖于极性相互作用. 模拟结果与实验数据较吻合. 相似文献
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Human immunodeficiency virus type 1 (HIV-1) integrase (IN) is an essential enzyme for splicing a viral DNA (vDNA) replica of its genome into host cell chromosomal DNA (hDNA) and has been recently recognized as a promising therapeutic target for developing anti-AIDS agents. The interaction between HIV-1 IN and vDNA plays an important role in the integration process of the virus. However, a detailed understanding about the mechanism of this interactions as well as the action of the anti-HIV drug raltegravir (RAL, approved by FDA in 2007) targeting HIV-1 IN in the inhibition of the vDNA strand transfer is still absent. In the present work, a molecular modeling study by combining homology modeling, molecular dynamics (MD) simulations with molecular mechanics Poisson-Boltzmann surface area (MM-PBSA), and molecular mechanics Generalized-Born surface area (MM-GBSA) calculations was performed to investigate the molecular mechanism of HIV-1 IN-vDNA interactions and the inhibition action of vDNA strand transfer inhibitor (INSTI) RAL. The structural analysis showed that RAL did not influence the interaction between vDNA and HIV-1 IN, but rather targeted a special conformation of HIV-1 IN to compete with host DNA and block the function of HIV-1 IN by forcing the 3'-OH of the terminal A17 nucleotide away from the three catalytic residues (Asp64, Asp116, and Glu152) and two Mg(2+) ions. Thus, the obtained results could be helpful for understanding of the integration process of the HIV-1 virus and provide some new clues for the rational design and discovery of potential compounds that would specifically block HIV-1 virus replication. 相似文献
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为了获得高活性、结构新颖的整合酶链转移(INST)抑制剂,本文采用Co MFA和Co MSIA两种方法对32个萘啶类INST抑制剂进行了三维定量构效关系研究,并建立了相关模型,其交叉验证系数分别为q~2=0. 809和q~2=0. 816,拟合验证系数分别为r~2=0. 998和r~2=0. 981,表明所建立的模型是可靠的且具有一定的预测能力。利用分子对接探讨小分子化合物与INST蛋白的相互作用模式,结果表明,萘啶类化合物主要通过疏水作用和氢键作用与INSTIs蛋白结合。最后通过分子动力学模拟进一步验证对接结果发现,对接的结合模式与分子动力学模拟得到的结果是一致的。本研究获得的综合模型和推论可以为开发有效的HIV INSTIs提供重要的理论信息。 相似文献