5,6-二氢-(9H)-吡唑[3,4-c]-1,2,4-三唑[4,3-a]吡啶类抑制剂的HQSAR研究

应用分子全息定量构效关系(HQSAR)分析方法,以5,6-二氢-(9H)-吡唑[3,4-c]-1,2,4-三唑[4,3-a]吡啶类抑制剂为研究对象,建立了一组对磷酸二酯酶4有抑制活性的化合物HQSAR模型,分析化合物活性与分子结构之间的关系.探讨了分子全息长度、分子碎片大小以及碎片区分参数对模型质量的影响.最优模型的交叉验证相关系数q2=0.628,非交叉验证相关系数r2=0.930,标准偏差SE=0.277.该模型具有较好的预测能力,对该类化合物性质的预测及进一步合成工作有指导意义.     

培氟沙星均三唑硫醚衍生物抗肝癌活性的CoMFA模型与分子设计

基于比较分子力场分析(CoMFA)方法建立24种培氟沙星均三唑硫醚衍生物抗肝癌活性(pM)的三维定量构效关系(3D-QSAR)。训练集中20个化合物用于建立预测模型,测试集10个化合物(含模板分子及新设计的5个分子)作为模型验证。已建立的3D-QSAR模型的交叉验证系数(R_cv²)、非交叉验证系数(R^₂)分别为0.705、0.940,说明所建模型具有较强的稳定性和良好的预测能力。该模型中立体场、静电场贡献率依次为74.8%、25.2%,表明影响抗肝癌活性(pM)的主要因素是取代基的疏水性和空间契合,其次是库仑力、氢键及配位。基于三维等势图,设计了5个具有较高抗肝癌活性的分子,有待医学实验验证。     

3-吡啶基醚类化合物的分子全息QSAR研究

采用分子全息定量构效关系(HQSAR, hologram quantitative structure-activity relationship)方法, 研究了28个3-吡啶基醚类化合物对乙酰胆碱α4β2受体的亲和性与它们的分子结构之间的关系, 讨论了分子碎片大小、分子碎片亚结构类型以及分子全息长度对QSAR的影响, 得到了较好的HQSAR模型, 模型的交叉验证系数平方q²＝0.670, 非交叉相关系数平方r²＝0.965, 偏差S＝0.093. 利用HQSAR的颜色编码, 对化合物中不同基团对亲和活性的影响进行了讨论, 对新配体的合成具有一定的指导作用.     

5-羧基苯并咪唑类HCV NS5B聚合酶抑制剂的HQSAR研究及分子设计

利用分子全息技术研究了129个5-羧基苯并咪唑类HCV NS5B聚合酶抑制剂的结构与活性之间的关系.讨论了分子碎片大小、碎片区分参数及全息长度对模型质量的影响.利用偏最小二乘法(partial least square,PLS)建立了一组以99个化合物为训练集的最优模型,该模型的交叉验证相关系数q~2=0.820,非交叉验证相关系数r~2=0.963,标准偏差SEE=0.213;用最优模型对由30个化合物组成的测试集进行预测,得到其相关系数r_(pred)~2=0.98,表明了该模型具有良好的预测能力及拟合能力.利用色码图对模型中不同原子及不同结构的贡献进行了解释,在此基础上根据最优HQSAR模型设计了几种具有良好抗HCV活性的苯并咪唑类HCV NS5B聚合酶抑制剂分子,为新型HCV NS5B聚合酶抑制剂的设计和优化提供了参考.     

多种类表面活性剂临界胶束浓度定量构效关系

表面活性剂的临界胶束浓度(CMC)是个非常重要的物质特性参数, CMC在研究表面活性剂的工业应用和生物利用方面发挥着关键作用. 本工作提出了一个新的拓扑指数—扩展距离矩阵, 建立了一个稳定的构效关系模型, 并对175种表面活性剂的临界胶束浓度进行了计算预测. 结果表明, 基于新的拓扑指数建立的构效关系模型计算临界胶束浓度能给出稳定可靠的预测结果, 其预测结果相关性系数R²(training set)=0.9295, 相对标准偏差ARD(training set)=8.20%, R²(testing set)=0.9257, ARD(testing set)=6.76%. 与文献中模型预测结果的对比表明, 本工作在稳定性和可靠性上均有显著改善.     

苯并咪唑类缓蚀剂的3D-QSAR研究及分子设计

采用比较分子场分析法(CoMFA)和比较分子相似性指数分析法(CoMSIA), 对苯并咪唑衍生物抗盐酸腐蚀的缓蚀性能进行了三维定量构效关系研究, 并使用留一法交叉验证手段对3D-QSAR模型的稳定性及预测能力进行了分析. 结果表明, 立体场、静电场和氢键供体场(电子给体)是影响苯并咪唑缓蚀剂缓蚀性能的主要因素; 所构建的CoMFA模型(q2=0.541, R2=0.996)和CoMSIA模型(q2=0.581, R2=0.987)均具有较好的统计学稳定性和预测能力. 基于3D-QSAR等势图设计出了几种具有较好缓蚀性能的苯并咪唑化合物, 为油气田新型缓蚀剂的研发提供了一种新思路.     

五元杂环并嘧啶类胸苷酸合成酶抑制剂的构效关系和分子对接

用比较分子场分析法(CoMFA)和比较分子相似性指数分析法(CoMSIA)研究了38个五元杂环并嘧啶衍生物类胸苷酸合成酶抑制剂的三维定量构效关系(3D-QSAR), 建立了相关预测模型. CoMFA和CoMSIA模型的交互验证相关系数q²分别为0.662和0.672、非交互验证相关系数R²分别为0.921和0.884、外部交互验证相关系数Q_ext²分别为0.85和0.81. 分子对接得到的结合模式与三维定量构效关系得到的结果一致. 结果表明这两种模型都具有良好的预测能力, 可应用于指导化合物的设计和结构修饰, 为进一步设计新型胸苷酸合成酶抑制剂提供了理论依据.     

具有除草活性的大环内酯类衍生物的定量构效关系

研究了一系列结构新颖的具有除草活性的大环内酯衍生物的定量构效关系(QSAR). 构建的比较分子力场分析(CoMFA)、比较分子近似指数分析(CoMSIA)和全息定量构效关系(HQSAR)分子模型的交叉验证系数r2cv均大于0.5, 非交叉验证系数r2都超过0.8, 表明获取的QSAR模型具有可信的预测能力. 对CoMFA、CoMSIA模型的三维(3D)等势图分析, 发现除了立体场和静电场外, 疏水场和氢键受体场也是影响大环内酯类化合物除草活性的重要因素. 构建的HQSAR模型的原子贡献图提示的结构改造信息与三维QSAR的结果基本一致. 利用CoMFA、CoMSIA模型提供的信息,对目前已合成的活性最高化合物B1-3进行分子结构改造, 预测结果发现部分化合物可能具有更好的除草活性.     

靛玉红类CDK1抑制剂的同源模建、分子对接及3D-QSAR研究

细胞周期蛋白依赖性激酶1的异常表达会导致G2期的停滞及多种肿瘤的发生,故CDK1近年来已成为一个理想的治疗靶点. 本文以细胞分裂调控蛋白2的同源体为模板,同源模建了CDK1的结构,并与靛玉红类小分子抑制剂进行分子对接. 分别运用三种叠合方法进行分子叠合,并在此基础上采用Sybyl 7.1中的比较分子场分析(CoMFA)模块及Discovery Studio 3.0中的三维定量构效关系(3D-QSAR)模块(以下简称为DS)分别建立了3D-QSAR模型. 其中,将分子对接叠合与公共骨架叠合联合运用的叠合方法所得3D-QSAR模型的评价参数是最佳的(CoMFA：q²=0.681,r²=0.909,r_pred.²=0.836; DS：q²=0.579,r²=0.971,r_pred.²=0.795,其中q²为交叉验证系数,r²为非交叉验证系数). 本文的研究结果在对靛玉红类小分子进行结构修饰设计出新的CDK1抑制剂方面,可提供重要的理论基础.     

基于遗传算法的Caco-2细胞穿透系数的研究

采用遗传算法研究了一系列药物分子的Caco-2细胞表观穿透系数(lgP_eff)和分子结构之间的关系. 基于51个化合物构成的训练集, 计算得到了一组效果较好的定量构效关系(QSAR)模型. 这些模型不仅具有较好的回归能力, 还能对预测集中的分子进行较好的预测. 在计算得到的精华种群中, 共有4个分子参数具有较高的出现频率, 它们分别是lgD(表观酯水分配系数)、r_gyr(回旋半径)、Shadow-Xlength(分子在X维上的投影长度)以及N_HBD(氢键给体数目).     

Predicting toxicity of benzene derivatives by molecular hologram derived quantitative structure–activity relationships (QSARS)

Holographic quantitative structure–activity relationship (HQSAR) is an emerging QSAR technique with the combined application of molecular hologram, which encodes the frequency of occurrence of various molecular fragment types, and the subsequent partial least squares (PLS) regression analysis. Based on molecular hologram, alignment-free QSAR models could be rapidly and easily developed with highly statistical significance and predictive ability. In this paper, the toxicity data for a series of 83 benzene derivatives to the autotrophic Chlorella vulgaris (IGC⁵⁰, negative logarithmic form of 6-h 50% population growth inhibition concentration in mmol/l) were subjected to HQSAR analysis and this resulted in a model with a high predictive ability. The robustness and predictive ability of the model were validated by “leave-one-out” (LOO) cross-validation procedure and an external testing set. The influence of fragment distinction parameters and fragment size on the quality of the HQSAR model have been also discussed.     

三苯胺类染料敏化太阳能电池能量转化效率的全息定量构效关系研究

研究构建了三苯胺类化合物分子结构与相应染料敏化太阳能电池能量转化效率(PCE)之间的全息定量构效关系(HQSAR)模型。当fragment distinction、fragment size、hologram length和principal components分别为“C、DA”、“4-7”、“199”和“6”时,可以获得最优HQSAR模型。采用外部测试集验证和留一交叉验证对所建立模型进行检验,外部测试集验证中CCC和 Q2F3分别为0.933和0.892,留一交叉验证中其q2cv和r2分别为0.791和0.902,表明所建立模型具有较好的拟合效果和预测能力。通过所建立HQSAR模型的分子贡献图可知,环戊并二噻吩基团的存在有利于提高PCE值,长烷基链的存在可能降低PCE值。     

Predicting toxicity of benzene derivatives by molecular hologram derived quantitative structure-activity relationships (QSARS)

Holographic quantitative structure-activity relationship (HQSAR) is an emerging QSAR technique with the combined application of molecular hologram, which encodes the frequency of occurrence of various molecular fragment types, and the subsequent partial least squares (PLS) regression analysis. Based on molecular hologram, alignment-free QSAR models could be rapidly and easily developed with highly statistical significance and predictive ability. In this paper, the toxicity data for a series of 83 benzene derivatives to the autotrophic Chlorella vulgaris (IGC50, negative logarithmic form of 6-h 50% population growth inhibition concentration in mmol/l) were subjected to HQSAR analysis and this resulted in a model with a high predictive ability. The robustness and predictive ability of the model were validated by "leave-one-out" (LOO) cross-validation procedure and an external testing set. The influence of fragment distinction parameters and fragment size on the quality of the HQSAR model have been also discussed.     

Quantitative structure-activity relationships for a series of selective estrogen receptor-beta modulators

The estrogen receptor-beta subtype (ERβ) is an attractive drug target for the development of novel therapeutic agents for hormone replacement therapy. Hologram quantitative structure-activity relationships (HQSAR) were conducted on a series of 6-phenylnaphthalene and 2-phenylquinoline derivatives, employing values of ERβ binding affinity. A training set of 65 compounds served to derive the models. The best statistical HQSAR model (q ²?=?0.73 and r ²?=?0.91) was generated using atoms, bonds, connections and donor and acceptor as fragment distinction parameters, and fragment size default (4–7) with hologram length of 199. The model was used to predict the binding affinity of an external test set of 16 compounds, and the predicted values were in good agreement with the experimental results. The final HQSAR model and the information obtained from 2D contribution maps should be useful for the design of novel ERβ modulators having improved affinity.     

A comparative study of quantitative structure-activity relationship methods based on gallic acid derivatives

By using hologram quantitative structure-activity relationship (HQSAR) and comparative molecular field analysis (CoMFA) methods, the relationships between the structures of 49 gallic acid derivatives and their analgesic activity have been investigated to yield statistically reliable models with considerable predictive power. The best HQSAR model was generated using atoms, bond and connectivity as fragment distinction parameters and fragment size 5-7 from a hologram length of 307 with 3 components. High conventional r2 (r2 = 0.825) and cross-validation r2 (r2(cv) = 0.726) values were obtained. CoMFA analyses varying lattice size and location, grid spacing, probe charges and using, Tripos standard and Indicator force field were performed. The best model was developed with 4 components using sp3-hybridized carbon atom with +1.0 charge as probe, grid spacing (2 A), lattice offset (1.0, 3.0, -2.5). The CoMFA model showed a conventional correlation coefficient r2 of 0.889 and across-validation r2(cv) equals to 0.633. The robustness and predictive ability of the HQSAR and CoMFA models have been validated by means of an external test set. The results indicate that both models possess high statistical quality in the prediction of analgesic potency of novel gallic acid analogs.     

Topomer CoMFA,HQSAR Studies and Molecular Docking of 2,5-Diketopiperazine Derivatives as Oxytocin Inhibitors

Topomer comparative molecular field analysis(Topomer Co MFA) and holographic quantitative structure-activity relationship(HQSAR) for 130 2,5-diketopiperazine derivatives were used to build a three-dimensional quantitative structure-activity relationship(3D-QSAR) model. The results show that the models have high predictive ability. For Topomer CoMFA, the cross-validated q~2 value is 0.710 and the non-cross-validated r~2 value is 0.834. The most effective HQSAR model shows that the cross-validation q~2 value is 0.700, the non-cross-validated r~2 value is 0.815, and the best hologram length value is 353 using connections and bonds as fragment distinctions. 50 highly active 2,5-diketopiperazine derivatives were designed based on the three-dimensional equipotential map and HQSAR color code map. Finally, the molecular docking method was also used to study the interactions of these new molecules by docking the ligands into the diketopiperazine active site, which revealed the likely bioactive conformations. This study showed that there are extensive interactions between the new molecule and Arg156, Arg122 residues in the active site of diketopiperazine. These results provide useful insights for the design of potent of the new 2,5-diketopiperazine derivatives.