主成分因子分析法对人Xa因子抑制剂n2 -芳酰氰胺类药物的QSAR研究。

Drug design and discovery Pub Date : 2002-01-01 DOI:10.3109/10559610213503

K. Roy, A. De, C. Sengupta

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引用次数: 9

摘要

人因子Xa抑制剂n2 -芳酰蒽酰胺的定量构效关系(QSAR)研究，最近由Yee等人(J. Med. Chem.)报道。， 43, 873-882)，采用主成分因子分析作为预处理步骤。研究表明，在对位(相对于酰胺键)存在给电子R2取代基有利于结合亲和力，而在间位R2取代基则降低亲和力。同样，具有较小体积和最佳亲水-亲脂平衡的供电子R1取代基(特别是甲基和甲氧基)有利于活性。研究进一步表明，吸电子的R3取代基对活性有害，而体积较大的R4取代基(特别是NHSO2Me基)则提高了活性。

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QSAR of human factor Xa inhibitor N2-aroylanthranilamides using principal component factor analysis.

Quantitative structure-activity relationship (QSAR) study of human factor Xa inhibitor N2-aroylanthranilamides, recently reported by Yee et al. (J. Med. Chem., 43, 873-882), has been performed using principal component factor analysis as the preprocessing step. The study reveals that presence of electron-donating R2 substituent at the para position (with respect to the amide linkage) is conducive to the binding affinity, whereas a meta R2 substituent decreases the affinity. Again, electron-donating R1 substituents with less bulk and optimum hydrophilic-lipophilic balance (particularly, methyl and methoxy groups) favor the activity. The study further suggests that electron-withdrawing R3 substituents are detrimental for the activity, whereas bulkier R4 substituents (particularly NHSO2Me group) increase the activity.

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Drug design and discovery

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