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A novel vector of topological and structural information for amino acids and its QSAR applications for peptides and analogues 被引量:2
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作者 LI ZhiLiang LI GenRong +9 位作者 SHU Mao SUN JiaYing YANG ShanBin MEI Hu ZHANG MengJun ZHOU Ping WU ShiRong CHEN GuoHua LU FengLin LU TingTing 《Science China Chemistry》 SCIE EI CAS 2008年第10期946-957,1021-1056,共48页
A new descriptor, called vector of topological and structural information for coded and noncoded amino acids (VTSA), was derived by principal component analysis (PCA) from a matrix of 66 topological and structural var... A new descriptor, called vector of topological and structural information for coded and noncoded amino acids (VTSA), was derived by principal component analysis (PCA) from a matrix of 66 topological and structural variables of 134 amino acids. The VTSA vector was then applied into two sets of peptide quantitative structure-activity relationships or quantitative sequence-activity modelings (QSARs/QSAMs). Molded by genetic partial least squares (GPLS), support vector machine (SVM), and immune neural network (INN), good results were obtained. For the datasets of 58 angiotensin converting enzyme inhibitors (ACEI) and 89 elastase substrate catalyzed kinetics (ESCK), the R 2, cross-validation R 2, and root mean square error of estimation (RMSEE) were as follows: ACEI, R cu 2 ?0.82, Q cu 2 ?0.77, E rmse?0.44 (GPLS+SVM); ESCK, R cu 2 ?0.84, Q cu 2 ?0.82, E rmse?0.20 (GPLS+INN), respectively. 展开更多
关键词 VECTOR of TOPOLOGICAL and STRUCTURAL information for coded and noncoded amino acids (VTSA) peptide QUANTITATIVE structure ACTIVITY relationship (pQSAR) molecular STRUCTURAL characterizing descriptors (MSCD) QUANTITATIVE sequence ACTIVITY modelings (qsams) angiotensin converting enzyme inhibitors (ACEI) ELASTASE substrate catalyzed kinetics (ESCK)
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