Identification of fructose 6-phosphate- and fructose 1-phosphate-binding residues in the regulatory protein of glucokinase

被引：54

作者：

Veiga-da-Cunha, M

Van Schaftingen, E

机构：

[1] Christian De Duve Inst Cellular Pathol, Physiol Lab, B-1200 Brussels, Belgium

[2] Univ Catholique Louvain, Physiol Chem Lab, B-1200 Brussels, Belgium

来源：

JOURNAL OF BIOLOGICAL CHEMISTRY | 2002年 / 277卷 / 10期

关键词：

D O I：

10.1074/jbc.M105984200

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Glucokinase is inhibited in the liver by a regulatory protein (GKRP) whose effects are increased by Fru-6-P and suppressed by Fru-1-P. To identify the binding site of these phosphate esters, we took advantage of the homology of GKRP to the isomerase domain of GlmS (glucosamine-6-phosphate synthase) and created 12 different mutants of rat GERP. Mutations of three residues predicted to bind to Fru-6-P resulted in proteins that were similar to5-fold (S110A) and 50-fold (S179A and K514A) less potent as inhibitors of glucokinase and had an at least 100-fold reduced affinity for the effectors. Mutation of another residue of the putative binding site (T109A) resulted in a 10-fold decrease in the inhibitory power and an inversion of the effect of sorbitol-6-P, a Fru-6-P analog. The replacement of Gly(107), a residue close to the binding site, by cysteine (as in GlmS and Xenopus GKRP) resulted in a protein that had 20 times more affinity for Fru-6-P and 30 times less affinity for Fru-1-P. These results are consistent with GKRP having one single binding site for phosphate esters. They also show that a missense mutation of GKRP can lead to a gain of function.

引用

页码：8466 / 8473

页数：8

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