Department of Chemistry and Biochemistry, University of California, San Diego, La Jolla, CA 92093, USA.
Institute for Memory Impairments and Neurological Disorders, University of California, Irvine, Irvine, CA 92697, USA.
ChemMedChem. 2021 Jun 7;16(11):1775-1787. doi: 10.1002/cmdc.202100111. Epub 2021 Mar 31.
Insulin-degrading enzyme (IDE) is a human mononuclear Zn -dependent metalloenzyme that is widely regarded as the primary peptidase responsible for insulin degradation. Despite its name, IDE is also critically involved in the hydrolysis of several other disparate peptide hormones, including glucagon, amylin, and the amyloid β-protein. As such, the study of IDE inhibition is highly relevant to deciphering the role of IDE in conditions such as type-2 diabetes mellitus and Alzheimer disease. There have been few reported IDE inhibitors, and of these, inhibitors that directly target the active-site Zn ion have yet to be fully explored. In an effort to discover new, zinc-targeting inhibitors of IDE, a library of ∼350 metal-binding pharmacophores was screened against IDE, resulting in the identification of 1-hydroxypyridine-2-thione (1,2-HOPTO) as an effective Zn -binding scaffold. Screening a focused library of HOPTO compounds identified 3-sulfonamide derivatives of 1,2-HOPTO as inhibitors of IDE (K values of ∼50 μM). Further structure-activity relationship studies yielded several thiophene-sulfonamide HOPTO derivatives with good, broad-spectrum activity against IDE that have the potential to be useful pharmacological tools for future studies of IDE.
胰岛素降解酶(IDE)是一种人类单核细胞 Zn 依赖性金属蛋白酶,被广泛认为是主要负责胰岛素降解的肽酶。尽管它的名字是这样,但 IDE 也在几种其他不同的肽类激素的水解中起着至关重要的作用,包括胰高血糖素、胰岛淀粉样多肽和淀粉样 β 蛋白。因此,研究 IDE 的抑制作用对于阐明 IDE 在 2 型糖尿病和阿尔茨海默病等疾病中的作用非常重要。目前报道的 IDE 抑制剂很少,其中直接针对活性位点 Zn 离子的抑制剂尚未得到充分探索。为了发现新的、针对锌的 IDE 抑制剂,我们对一个约 350 个金属结合药效团的库进行了 IDE 筛选,结果发现 1-羟基吡啶-2-硫酮(1,2-HOPTO)是一种有效的 Zn 结合支架。对 HOPTO 化合物的聚焦文库进行筛选,发现 1,2-HOPTO 的 3-磺酰胺衍生物是 IDE 的抑制剂(K 值约为 50 μM)。进一步的构效关系研究得到了几种噻吩磺酰胺 HOPTO 衍生物,它们对 IDE 具有良好的广谱活性,有可能成为未来 IDE 研究的有用药理学工具。
