糖原磷酸化酶b与一种新型强效抑制剂烷基二氢吡啶二羧酸化合物的结构

The structure of glycogen phosphorylase b with an alkyldihydropyridine-dicarboxylic acid compound, a novel and potent inhibitor.

作者信息

Zographos S E, Oikonomakos N G, Tsitsanou K E, Leonidas D D, Chrysina E D, Skamnaki V T, Bischoff H, Goldmann S, Watson K A, Johnson L N

机构信息

Institute of Biological Research and Biotechnology, The National Hellenic Research Foundation 48, vas Constantinou Avenue, Athens, 11635, Greece.

出版信息

Structure. 1997 Nov 15;5(11):1413-25. doi: 10.1016/s0969-2126(97)00292-x.

DOI:10.1016/s0969-2126(97)00292-x

PMID:9384557

Abstract

BACKGROUND

In muscle and liver, glycogen concentrations are regulated by the reciprocal activities of glycogen phosphorylase (GP) and glycogen synthase. An alkyl-dihydropyridine-dicarboxylic acid has been found to be a potent inhibitor of GP, and as such has potential to contribute to the regulation of glycogen metabolism in the non-insulin-dependent diabetes diseased state. The inhibitor has no structural similarity to the natural regulators of GP. We have carried out structural studies in order to elucidate the mechanism of inhibition.

RESULTS

Kinetic studies with rabbit muscle glycogen phosphorylase b (GPb) show that the compound (-)(S)-3-isopropyl 4-(2-chlorophenyl)-1,4-dihydro-1-ethyl-2-methyl-pyridine-3,5, 6-tricarboxylate (Bay W1807) has a Ki = 1.6 nM and is a competitive inhibitor with respect to AMP. The structure of the cocrystallised GPb-W1807 complex has been determined at 100K to 2.3 A resolution and refined to an R factor of 0.198 (Rfree = 0.287). W1807 binds at the GPb allosteric effector site, the site which binds AMP, glucose-6-phosphate and a number of other phosphorylated ligands, and induces conformational changes that are characteristic of those observed with the naturally occurring allosteric inhibitor, glucose-6-phosphate. The dihydropyridine-5,6-dicarboxylate groups mimic the phosphate group of ligands that bind to the allosteric site and contact three arginine residues.

CONCLUSIONS

The high affinity of W1807 for GP appears to arise from the numerous nonpolar interactions made between the ligand and the protein. Its potency as an inhibitor results from the induced conformational changes that lock the enzyme in a conformation known as the T' state. Allosteric enzymes, such as GP, offer a new strategy for structure-based drug design in which the allosteric site can be exploited. The results reported here may have important implications in the design of new therapeutic compounds.

摘要

背景

在肌肉和肝脏中，糖原浓度受糖原磷酸化酶（GP）和糖原合酶的相互作用调节。已发现一种烷基二氢吡啶二羧酸是GP的有效抑制剂，因此有可能在非胰岛素依赖型糖尿病疾病状态下对糖原代谢的调节起作用。该抑制剂与GP的天然调节剂没有结构相似性。我们进行了结构研究以阐明抑制机制。

结果

用兔肌肉糖原磷酸化酶b（GPb）进行的动力学研究表明，化合物（-）（S）-3-异丙基4-（2-氯苯基）-1,4-二氢-1-乙基-2-甲基吡啶-3,5,6-三羧酸酯（Bay W1807）的Ki = 1.6 nM，是AMP的竞争性抑制剂。在100K下以2.3 Å分辨率测定了共结晶的GPb-W1807复合物的结构，并将其精修至R因子为0.198（Rfree = 0.287）。W1807结合在GPb变构效应物位点，该位点结合AMP、6-磷酸葡萄糖和许多其他磷酸化配体，并诱导出与天然存在的变构抑制剂6-磷酸葡萄糖所观察到的构象变化特征相同的构象变化。二氢吡啶-5,6-二羧酸基团模拟与变构位点结合并接触三个精氨酸残基的配体的磷酸基团。