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Characterization of Novel Dipeptidyl Peptidase-IV Inhibitory Peptides from Soft-Shelled Turtle Yolk Hydrolysate Using Orthogonal Bioassay-Guided Fractionations Coupled with In Vitro and In Silico Study

机译:使用正交生物测定引导分级与体外和硅研究中的软壳龟蛋白水解产物的新型二肽肽肽酶-IV抑制肽的表征

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摘要

Five novel peptides (LPLF, WLQL, LPSW, VPGLAL, and LVGLPL) bearing dipeptidyl peptidase IV (DPP-IV) inhibitory activities were identified from the gastrointestinal enzymatic hydrolysate of soft-shelled turtle yolk (SSTY) proteins. Peptides were isolated separately using reversed-phase (RP) chromatography in parallel with off-line strong cation exchange (SCX) chromatography followed by liquid chromatography-tandem mass spectrometry (LC-MS/MS) analysis to determine sequences. Among these peptides, LPSW showed the highest DPP-IV inhibitory activity with an IC50 value of 269.7 ± 15.91 µM. The results of the pre-incubation experiment and the kinetic study of these peptides indicated that WLQL is a true inhibitor and its inhibition toward DPP-IV is of an uncompetitive model, while LPLF, LPSW, and VPGLAL are real-substrates and competitive inhibitors against DPP-IV. The DPP-IV inhibitory peptides derived from SSTY hydrolysate in study are promising in the management of hyperglycemia in Type 2 diabetes.
机译:从软壳龟蛋白(SSTY)蛋白的胃肠酶水解产物鉴定了五种新型肽(LPLF,WLQL,LPSW,VPGLAL和LVGLPL)含有二肽肽酶IV(DPP-IV)的抑制活性。使用反相(RP)色谱分别与离线强阳离子交换(SCX)色谱分别分别分离肽,然后用液相色谱 - 串联质谱(LC-MS / MS)分析来确定序列。在这些肽中,LPSW显示出最高的DPP-IV抑制活性,IC50值为269.7±15.91μm。预孵育实验结果和这些肽的动力学研究表明,WLQL是真正的抑制剂,其对DPP-IV的抑制作用是非竞争力的模型,而LPLF,LPSW和VPGLAL是实际基板和竞争性抑制剂DPP-IV。在研究中衍生自SSTY水解产物的DPP-IV抑制肽在2型糖尿病中的高血糖症的管理中是有前途的。

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