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Divergent effects of compounds on the hydrolysis and transpeptidation reactions of γ-glutamyl transpeptidase

机译:化合物对γ-谷氨酰转肽酶水解和转肽反应的不同作用

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A novel class of inhibitors of the enzyme γ-glutamyl transpeptidase (GGT) were evaluated. The analog OU749 was shown previously to be an uncompetitive inhibitor of the GGT transpeptidation reaction. The data in this study show that it is an equally potent uncompetitive inhibitor of the hydrolysis reaction, the primary reaction catalyzed by GGT in vivo. A series of structural analogs of OU749 were evaluated. For many of the analogs, the potency of the inhibition differed between the hydrolysis and transpeptidation reactions, providing insight into the malleability of the active site of the enzyme. Analogs with electron withdrawing groups on the benzosulfonamide ring, accelerated the hydrolysis reaction, but inhibited the transpeptidation reaction by competing with a dipeptide acceptor. Several of the OU749 analogs inhibited the transpeptidation reaction by slow onset kinetics, similar to acivicin. Further development of inhibitors of the GGT hydrolysis reaction is necessary to provide new therapeutic compounds.
机译:评价了新型的γ-谷氨酰转肽酶(GGT)抑制剂。先前显示类似物OU749是GGT转肽反应的非竞争性抑制剂。这项研究中的数据表明,它是水解反应的一种同样有效的非竞争性抑制剂,水解反应是GGT在体内催化的主要反应。评估了OU749的一系列结构类似物。对于许多类似物,在水解反应和转肽反应之间抑制的效力是不同的,从而提供了对酶活性位点可塑性的了解。在苯甲磺酰胺环上具有吸电子基团的类似物,加速了水解反应,但通过与二肽受体竞争而抑制了转肽反应。某些OU749类似物通过缓慢的动力学起抑制转肽反应的作用,类似于阿西维奇。为了提供新的治疗化合物,必须进一步开发GGT水解反应抑制剂。

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