Imidazole-derived 2-[N-carbamoylmethyl-alkylamino]acetic acids, substrate-dependent modulators of insulin-degrading enzyme in amyloid-β hydrolysis

咪唑衍生的 2-[N-氨基甲酰甲基-烷基氨基]乙酸,淀粉样β蛋白水解中胰岛素降解酶的底物依赖性调节剂

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作者:Julie Charton, Marion Gauriot, Qing Guo, Nathalie Hennuyer, Xavier Marechal, Julie Dumont, Malika Hamdane, Virginie Pottiez, Valerie Landry, Olivier Sperandio, Marion Flipo, Luc Buee, Bart Staels, Florence Leroux, Wei-Jen Tang, Benoit Deprez, Rebecca Deprez-Poulain

Abstract

Insulin degrading enzyme (IDE) is a highly conserved zinc metalloprotease that is involved in the clearance of various physiologically peptides like amyloid-beta and insulin. This enzyme has been involved in the physiopathology of diabetes and Alzheimer's disease. We describe here a series of small molecules discovered by screening. Co-crystallization of the compounds with IDE revealed a binding both at the permanent exosite and at the discontinuous, conformational catalytic site. Preliminary structure-activity relationships are described. Selective inhibition of amyloid-beta degradation over insulin hydrolysis was possible. Neuroblastoma cells treated with the optimized compound display a dose-dependent increase in amyloid-beta levels.

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