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潜在抗糖尿病药物的设计:多种糖原磷酸化酶的β-D-葡萄糖类似物抑制剂的实验研究

The design of potential antidiabetic drugs: experimental investigation of a number of beta-D-glucose analogue inhibitors of glycogen phosphorylase.

作者信息

Oikonomakos N G, Kontou M, Zographos S E, Tsitoura H S, Johnson L N, Watson K A, Mitchell E P, Fleet G W, Son J C, Bichard C J

机构信息

National Hellenic Research Foundation, Athens, Greece.

出版信息

Eur J Drug Metab Pharmacokinet. 1994 Jul-Sep;19(3):185-92. doi: 10.1007/BF03188920.

Abstract

alpha-D-glucose is a weak inhibitor (Ki = 1.7 mM) of glycogen phosphorylase (GP) and acts as physiological regulator of hepatic glycogen metabolism; it binds to GP at the catalytic site and stabilizes the inactive T state of the enzyme promoting the action of protein phosphatase 1 and stimulating glycogen synthase. The three-dimensional structures of T state rabbit muscle GPb and the GPb-alpha-D-glucose complex have been exploited in the design of better regulators of GP that could shift the balance between glycogen synthesis and glycogen degradation in favour of the former. Close examination of the catalytic site with alpha-D-glucose bound shows that there is an empty pocket adjacent to the beta-1-C position. beta-D-glucose is a poorer inhibitor (Ki = 7.4 mM) than alpha-D-glucose, but mutarotation has prevented the binding of beta-D-glucose in T state GP crystals. A series of beta-D-glucose analogues has been designed and tested in kinetic and crystallographic experiments. Several compounds have been discovered that have an increased affinity for GP than the parent compound.

摘要

α-D-葡萄糖是糖原磷酸化酶(GP)的一种弱抑制剂(Ki = 1.7 mM),并作为肝脏糖原代谢的生理调节剂;它在催化位点与GP结合,稳定酶的无活性T态,促进蛋白磷酸酶1的作用并刺激糖原合酶。T态兔肌肉GPb和GPb-α-D-葡萄糖复合物的三维结构已被用于设计更好的GP调节剂,这些调节剂可以改变糖原合成与糖原降解之间的平衡,使其有利于前者。对结合α-D-葡萄糖的催化位点进行仔细检查发现,在β-1-C位置附近有一个空口袋。β-D-葡萄糖是一种比α-D-葡萄糖更弱的抑制剂(Ki = 7.4 mM),但变旋作用阻止了β-D-葡萄糖在T态GP晶体中的结合。已经设计了一系列β-D-葡萄糖类似物,并在动力学和晶体学实验中进行了测试。已发现几种化合物对GP的亲和力比母体化合物有所增加。

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