Inhibitory mechanism of carboxymethyl chitosan-lotus seedpod oligomeric procyanidin nanoparticles on dietary advanced glycation end products released from glycated casein during digestion

被引:3
作者
Wu, Qian [1 ]
Zhang, Fen [1 ]
Wang, Yaxiong [1 ]
Yan, Jia [1 ]
Zhou, Chen
Xu, Yang [1 ]
Xu, Jianhua [2 ]
Shi, Lin [3 ]
Xiong, He [3 ]
Feng, Nianjie [1 ]
机构
[1] Hubei Univ Technol, Hubei Key Lab Ind Microbiol, Natl 111 Ctr Cellular Regulat & Mol Pharmaceut, Key Lab Fermentat Engn,Minist Educ, Wuhan 430068, Hubei, Peoples R China
[2] Pinyuan Suizhou Modern Agr Dev Co LTD, Suizhou 441300, Hubei, Peoples R China
[3] Wuhan Caidian Dist Publ Inspect & Testing Ctr, Wuhan 430100, Hubei, Peoples R China
基金
中国国家自然科学基金;
关键词
Lotus seedpod oligomeric procyanidins (LSOPC); Carboxymethyl chitosan-lotus seedpod oligomeric procyanidin nanoparticles (CMC-LSOPC NPs); Advanced glycation end products (AGEs); Gastrointestinal digestion; Stability Inhibitory mechanism; IN-VITRO DIGESTION; ANTIOXIDANT ACTIVITY; TEA CATECHINS; DELIVERY; FOODS;
D O I
10.1016/j.foodres.2023.113412
中图分类号
TS2 [食品工业];
学科分类号
0832 ;
摘要
Lotus seedpod oligomeric procyanidins (LSOPC) are potent inhibitors of advanced glycation end products (AGEs), whose gastrointestinal susceptibility to degradation limits their use in vivo. In this study, carboxymethyl chitosan-lotus seedpod oligomeric procyanidin nanoparticles (CMC-LSOPC NPs) were constructed with a binding ratio of 1:6.51. CMC-LSOPC NPs significantly inhibited the release of AGEs from glycated casein (G-CS) during digestion, increasing the inhibition rate by 25.76% in the gastric phase and by 14.33% in the intestinal phase compared with LSOPC alone. To further investigate the inhibition mechanism, fluorescence microscopy, scanning electron microscopy and FTIR were used to find that CMC-LSOPC NPs could form cohesions to encapsulate G-CS in the gastric phase and hinder G-CS hydrolysis. In the intestinal phase, LSOPC was targeted for release and bound to trypsin through hydrophobic interactions and hydrogen bonding, resulting in protein peptide chain rearrangement, changes in secondary structure and significant reduction in trypsin activity. In addition, CMC-LSOPC NPs increased the antioxidant capacity of digestive fluid and could reduce the oxidative stress in the gastrointestinal tract caused by the release of AGEs. It's the first time that CMC-LSOPC NPs were constructed to enhance the stability of LSOPC during digestion and explain the mechanism by which CMC-LSOPC NPs inhibit the release of AGEs from G-CS in both stomach and intestine. This finding will present a novel approach for reducing AGEs during gastrointestinal digestion.
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页数:12
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