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曲亭菲,赵前程,李双双,韩明哲,李嘉欣,马永生.仿刺参胶原蛋白源二肽基肽酶抑制肽虚拟筛选及分子对接研究[J].食品安全质量检测学报,2023,14(2):9-17

仿刺参胶原蛋白源二肽基肽酶抑制肽虚拟筛选及分子对接研究

Virtual screening and molecular docking of dipeptidyl peptidase-IV inhibitory peptides derived from collagen of Apostichopus japonicus

投稿时间：2022-11-14 修订日期：2023-01-06

DOI：

中文关键词: 仿刺参虚拟酶解分子对接生物活性肽二肽基肽酶 Ⅱ型糖尿病

英文关键词:Apostichopus japonicus enzymatic hydrolysis in silico molecular docking bioactive peptides dipeptidyl peptidase-IV type Ⅱ diabetes

基金项目:国家重点研发计划项目(2020YFD0900704)、辽宁省教育厅科技项目(DL202002 )

作者	单位
曲亭菲	大连海洋大学食品科学与工程学院
赵前程	大连海洋大学食品科学与工程学院
李双双	大连鑫玉龙海洋生物种业科技股份有限公司
韩明哲	大连海洋大学食品科学与工程学院
李嘉欣	大连海洋大学食品科学与工程学院
马永生	大连海洋大学食品科学与工程学院

Author	Institution
QU Ting-Fei	College of Food Science and Engineering, Dalian Ocean University
ZHAO Qian-Cheng	College of Food Science and Engineering, Dalian Ocean University
LI Shuang-Shuang	Dalian Xinyulong Marine Organisms Seed Industry Technology Co., Ltd
HAN Ming-Zhe	College of Food Science and Engineering, Dalian Ocean University
LI Jia-Xin	College of Food Science and Engineering, Dalian Ocean University
MA Yong-Sheng	College of Food Science and Engineering, Dalian Ocean University

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中文摘要:

目的采用生物信息学和分子对接方法筛选仿刺参胶原蛋白来源的二肽基肽酶(dipeptidyl peptidase-IV, DPP-IV)抑制肽。方法以仿刺参胶原蛋白序列为对象，进行生物信息学分析和计算机辅助虚拟酶解, 基于生物毒性、致敏性、水溶性及吸收、分配、代谢、排泄及毒性(absorption, distribution, metabolism, excretion, toxicity, ADMET)预测, 筛选得到6条具有潜在生物活性的寡肽, 氨基酸序列分别为CD、CQ、CS、GR、SM、MDG, 进一步通过分子对接分析肽段与DPP-Ⅳ的结合活性, 并分析其结合位点及方式。结果生物信息学分析表明仿刺参胶原蛋白是生物活性肽的潜在优良来源, 经木瓜蛋白酶、碱性蛋白酶及模拟胃肠道虚拟水解后能够释放出DPP-Ⅳ抑制肽; 分子对接表明俩条新肽段CS、SM通过氢键、疏水相互作用分别与DPP-IV的S1、S2活性口袋结合。结论本研究提供了一种快速筛选刺参胶原蛋白中DPP-IV抑制肽的方法。

英文摘要:

Objective To screen the dipeptidyl peptidase-IV (DPP-IV) inhibitory peptides derived from Apostichopus japonicus (A. japonicus) collagen by the bioinformatics and molecular docking method. Methods The sequence of A. japonicus collagen was analyzed and virtual enzymolysised by bioinformatics in silico. Based on the prediction of biological toxicity, sensitization, solubility, absorption, distribution, metabolism, excretion, and toxicity (ADMET), 6 oligopeptides with potential biological activity were screened out, and their amino acid sequences were CD, CQ, CS, GR, SM, and MDG, respectively. In addition, the binding activity of these peptides with DPP-IV were further analyzed by molecular docking, and their binding sites and binding modes were analyzed. Results Bioinformatics analysis showed that A. japonicus collagen was a potential excellent bioactive peptides source, after hydrolyzed by papain, subtilisin, and simulated gastrointestinal digestion, DPP-IV inhibitory peptides could released. The results of molecular docking indicated that 2 new peptides CS and SM could bound to S1 and S2 active pockets of DPP-IV with hydrogen bondings and hydrophobic interactions, respectively. Conclusion This study provids a method to quickly screen DPP-IV inhibitory peptides from A. japonicus collagen.

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