Enhanced stability of oral insulin in targeted peptide ligand trimethyl chitosan nanoparticles against trypsin

被引:29
|
作者
Chen, Jiexiu [1 ]
Liu, Chong [1 ]
Shan, Wei [1 ]
Xiao, Zhijian [1 ]
Guo, Han [1 ]
Huang, Yuan [1 ]
机构
[1] Sichuan Univ, West China Sch Pharm, Minist Educ, Key Lab Drug Targeting & Drug Delivery Syst, Chengdu 610041, Peoples R China
关键词
Camostat mesylate; CSKSSDYQC peptide; insulin; oral delivery system; TMC; Ussing chamber; MUCOUS/GLYCOCALYX LAYERS; PROTEASE INHIBITION; USSING CHAMBER; IN-VITRO; ABSORPTION; DELIVERY; DEGRADATION; PERMEATION; PROTEINS; VIVO;
D O I
10.3109/02652048.2015.1065920
中图分类号
O69 [应用化学];
学科分类号
081704 ;
摘要
Oral insulin delivery is often limited by protease degradation. 2-(Dimethylamino)-2-oxoethyl 4-(4-guanidinobenzoyloxy)phenylacetate methanesulphonate (Camostat mesylate) is reported to have the ability to inhibit trypsin activity, which is the main protease responsible for protein degradation. This study attempted to form a novel nanoparticle by covalently conjugating 4-(2-(2-aminoethylamino)-2-oxoethyl) phenyl 4-guanidinobenzoyloxy (FOY-251), an active derivative of camostat mesylate, to the backbone of poly (gamma-glutamic acid) (gamma-PGA), in order to improve insulin stability against protease. Goblet cell targeting CSKSSDYQC (CSK) peptide was demonstrated to effectively improve the epithelial absorption of insulin. Therefore, the novel nanoparticle was prepared by mixing cationic peptide modified trimethyl chitosan (TMC-CSK) with anionic gamma PGA-FOY conjugate using multi-ion crosslinked method. Results showed that not only the gamma PGA-FOY conjugate but also the prepared novel nanoparticle could inhibit trypsin activity both in vitro environment and on the intestinal mucosal surface. This study would be beneficial for peptide modified nanoparticles in oral insulin delivery.
引用
收藏
页码:632 / 641
页数:10
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