HEPT类HIV-1逆转录酶衍生物的CoMFA、CoMSIA及HQSAR分析

采用比较分子力场分析法(CoMFA)、比较分子相似因子分析法(CoMSIA)和分子全息定量结构关系(HQSAR)对1-[(2-羟乙氧)甲基]-6-苯硫基胸腺嘧啶(HEPT)类衍生物进行了分子活性构象选择、分子叠合、空间力场范围建立以及相应3D-QSAR模型建立。结果表明:该法所建模型对此类化合物具有良好的预测能力。CoMFA模型显示,交叉验证系数(q2)为0.565,非交互验证系数(r2)为0.892;CoMSIA模型显示,最佳q2为0.636,r2为0.953;最佳的HQSAR模型显示,q2为0.876,r2为0.929,最佳全息长度为97。根据三维等势图和HQSAR色码图设计了7个有较高活性的HEPT类化合物。

Proposal and evaluation of a new norm index-based QSAR model to predict pEC50 and pCC50 activities of HEPT derivatives

The search and development of anti-HIV drugs is currently one of the most urgent tasks of pharmacological studies. In this work, a quantitative structure-activity relationship （QSAR） model based on some new norm indexes, was obtained to a series of more than 150 HEPT derivatives （1-[（2-hydroxyethoxy）methyl]-6-（phenylthio）thymine） to find their pEC50 （the required effective concentration to achieve 50% protection of MT-4 cells against the cytopathic effect of virus） and pCC50 （the required cytotoxic concentration to reduce visibility of 50% mock infected cell） activities. The model efficiencies were then validated using the leave-one-out cross validation （LOO-CV） and y- randomization test. Results indicated that this new model was efficient and could provide satisfactory results for prediction of pECso and pCC50 with the higher R2 train and the higher Rt2est. By using the leverage approach, the applicability domain of this model was further investigated and no response outlier was detected for HEFT derivatives involved in this work. Comparison results with reference methods demonstrated that this new method could result in significant improvements for predicting pEC50 and pCC50 of anti-HIV HEPT derivatives. Moreover, results shown in this present study suggested that these two absolutely different activities pECso and pCC50 of anti-HIV HEPT derivatives could be predicted well with a totally similar QSAR model, which indicated that this model mizht have the potential to be further utilized for other biological activities of HEFT derivatives.

新型HIV逆转录酶和整合酶双靶点抑制剂的虚拟筛选

目的构建3-OH HEPT类针对HIV逆转录酶非核苷类抑制剂作用靶点和整合酶的双靶点抑制剂[RT(NNRTI)/IN]药效团模型,对中药化学数据库(TCMD)进行搜索,寻找潜在的新型HIV双靶点抑制剂。方法从已知的3-OH HEPT类HIVRT(NNRTI)/IN双靶点抑制剂出发,构建药效团模型,基于药效团模型和Lipinski五规则对TCMD进行筛选,发现新的抗HIV双靶点抑制剂。结果构建的药效团模型包括6个药效特征基团,以符合6个药效特征基团中任意5个为条件,在测试集数据库中验证性搜索命中全部16个化合物,检出率达到了100%。利用所建的六点药效团模型和Lipinski五规则对TCMD筛选,得到符合条件的化合物229个,其中包含已知的抗HIV活性化合物。结论建立的药效团模型和筛选策略为后续研究打下了较好的基础。

HEPT 类似物的电子结构与抗 HIV 活性的关系研究

目的:为了研究HEPT 类似物的电子结构与其抗HIV 活性的关系。方法:应用分子力学MM+方法,半经验量子化学MNDO 法计算了23个HEPT 类似物的优势构象和电子结构,结合数理方法得到了两个定量构效方程:(1)log1/C=5.138+0.00005823I_(C-C)+0.00004894E_e+3.747Q_(13);(2)ClogP=5.271+0.0001363I_(C-C)+0.0001134E_e-10.86Q_(S13);结果:(1)HEPT 类似物的两个苯环作为两个核的核与核之间相互作用I_(C-C)和分子总电子能E_e 是影响其log1/C 与ClogP 的主要因素,核与核之间的相互作用越强,总电子能越高,则其疏水参数和其抗HIV 活性也越强。(2)13号原子上取代基的净电荷Q_(S13)越大时,ClogP 越小。当13号原子的净电荷Q_(13)越多,其抗HIV 活性则越强。结论:HEPT 类似物的抗HIV 活性与化合物的核与核之间相互作用、总电子能及13号位的原子的净电荷成正比。

应用随机共振研究一组抗癌药物定量结构活性相关

提出了一种基于随机共振理论的定量构效关系研究方法。随机共振现象中存在着将噪声的能量转移给信号,从而提高信号信噪比的机制,是一种处理噪声信号的有效方法。本文将随机共振算法应用于一组抗艾滋病药物的定量构效关系研究,以普遍存在于分子结构描述子之中的误差和冗余变量为噪声,而将与所研究化合物活性之间相关性较好的分子结构描述子作为信号,通过优化非线性系统的参数,实现了随机共振,达到了抑制误差、增强信号的目的。所建四变量模型的统计特性为：n=34,R^2=0.9601,s=0.29,Q^2=0.9508,F=168.62。结果表明,随机共振方法是一种提高定量构效关系模型性能的有效途径。