STRUCTURE-BASED DESIGN OF INHIBITORS OF PURINE NUCLEOSIDE PHOSPHORYLASE .3. 9-ARYLMETHYL DERIVATIVES OF 9-DEAZAGUANINE SUBSTITUTED ON THE METHYLENE GROUP

被引：59

作者：

ERION, MD

NIWAS, S

ROSE, JD

ANANTHAN, S

ALLEN, M

SECRIST, JA

BABU, YS

BUGG, CE

GUIDA, WC

EALICK, SE

MONTGOMERY, JA

机构：

[1] BIOCRYST PHARMACEUT INC,BIRMINGHAM,AL 35244

[2] SO RES INST,BIRMINGHAM,AL 35255

[3] UNIV ALABAMA,CTR MACROMOLEC CRYSTALLOG,BIRMINGHAM,AL 35294

[4] CIBA GEIGY CORP,DIV PHARMACEUT,SUMMIT,NJ 07901

来源：

JOURNAL OF MEDICINAL CHEMISTRY | 1993年 / 36卷 / 24期

关键词：

D O I：

10.1021/jm00076a004

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

X-ray crystallography and computer-assisted molecular modeling (CAMM) studies aided in the design of a potent series of mammalian purine nucleoside phosphorylase (PNP) inhibitors. Enhanced potency was achieved by designing substituted 9-(arymethyl)-9-deazaguanine analogs that interact favorably with all three of the binding subsites of the PNP active site, namely the purine binding site, the hydrophobic pocket, and the phosphate binding site. The most potent PNP inhibitor prepared during our investigation, (S)-9-[1-(3-chlorophenyl)-2-carboxyethyl]-9-deazaguanine (18b), was shown to have an IC50 of 6 nM, whereas the corresponding (R)-isomer was 30-fold less potent.

引用

页码：3771 / 3783

页数：13

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