Stabilized β‑Hairpin Peptide Inhibits Insulin Degrading Enzyme YangDan QinWeirong ShiXiaodong ZhuBili XieMingsheng ZhaoHui TengBin WuYujie ZhaoRongtong YinFeng RenPeigen LiuLizhong LiZigang 2018 Insulin-degrading enzyme (IDE) plays a critical role in both the proteolytic degradation and inactivation of insulin. The exploration of novel IDE inhibitors could aid in the study of novel therapeutics for type-2 diabetes. Herein, we report a hypothesized stabilized β-hairpin peptide that can efficiently inhibit the enzymatic activity of IDE. The resulting stabilized peptide <b>B35</b> is demonstrated to activate the AKT phosphorylation pathway in skeletal muscle cells and is shown to slow insulin degradation. An 80 mg kg<sup>–1</sup> intraperitoneal (i.p.) injection of the stabilized β-hairpin peptide <b>B35</b> is demonstrated to improve glucose tolerance during an oral glucose tolerance test in obese mouse model. We note that this stabilized peptide exhibited negligible cytotoxicity in both <i>in vitro</i> and <i>in vivo</i> assays, even at high concentrations (300 μM). This study suggests that IDE peptide inhibitors could function as potentially meaningful candidates for the development of type-2 diabetes therapeutics.