The synthesis of novel bisphosphonates as inhibitors of phosphoglycerate kinase (3-PGK)

被引:43
作者
Caplan, NA
Pogson, CI
Hayes, DJ
Blackburn, GM
机构
[1] Univ Sheffield, Dept Chem, Sheffield S3 7HF, S Yorkshire, England
[2] Glaxo Wellcome Inc, Stevenage, Herts, England
来源
JOURNAL OF THE CHEMICAL SOCIETY-PERKIN TRANSACTIONS 1 | 2000年 / 03期
关键词
D O I
10.1039/a906507e
中图分类号
O62 [有机化学];
学科分类号
070303 ; 081704 ;
摘要
A series of conformationally-restrained analogues of 1,3-bisphospho-D-glyceric acid (1,3-BPG) 1 has been synthesised for use as inhibitors of 3-PGK (E.C. 2.7.2.3). These compounds have non-scissile phosphonate linkages and also incorporate alpha-halogen substituents to make them isopolar and isosteric mimics of the natural substrate. A monocyclic aryl core between the two phosphoryl centres provides both a rigid framework linking these moieties and loci for further substitution. The compounds were tested against human 3-PGK and found to be good competitive inhibitors. alpha-Fluorination of the phosphonic acids increased the affinity for the enzyme into the submicromolar range. Correlation of IC50 data with pK(a3) and pK(a4) values indicates that the acidity of the phosphoryl group exerts a strong influence on protein binding.
引用
收藏
页码:421 / 437
页数:17
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