Acid-Resistant Mesoporous Metal-Organic Frameworks as Carriers for Targeted Hypoglycemic Peptide Delivery: Peptide Encapsulation, Release, and Bioactivity

被引:2
|
作者
Liu, Weiwei [1 ]
Ma, Ruolan [1 ]
Lu, Shiyi [1 ]
Wen, Yangyang [2 ]
Li, Hongyan [1 ]
Wang, Jing [1 ]
Sun, Baoguo [1 ]
Sun, Baoguo [1 ]
机构
[1] Beijing Technol & Business Univ BTBU, Sch Food & Hlth, China Canada Joint Lab Food Nutr & Hlth Beijing, Beijing 100048, Peoples R China
[2] Beijing Technol & Business Univ BTBU, Coll Chem & Mat Engn, Beijing 100048, Peoples R China
基金
中国国家自然科学基金; 中国博士后科学基金;
关键词
metal-organic framework; NU-1000; LDLQR; oral delivery; intestinal release; INSULIN; NANOPARTICLES; THERAPEUTICS; PERMEATION;
D O I
10.1021/acsami.2c18452
中图分类号
TB3 [工程材料学];
学科分类号
0805 ; 080502 ;
摘要
Oral administration of bioactive peptides with alpha- glucosidase inhibitory activities is a promising strategy for diabetes mellitus. The wheat germ peptide Leu-Asp-Leu-Gln-Arg (LDLQR) has been previously proven to inhibit the activity of alpha-glucosidase efficiently. However, it is still difficult to transport the peptide to the intestine completely due to the harsh condition of the stomach. Herein, an acid-resistant zirconium-based metal- organic framework, NU-1000, was used to immobilize LDLQR with a high encapsulation capacity (92.72%) and encapsulation efficiency (44.08%) in only 10 min. The in vitro release results showed that the acid-stable NU-1000 not only effectively protected LDLQR from degradation in the presence of stomach acid and pepsin effectively but also ensured the release of encapsulated LDLQR under simulated intestinal conditions. Furthermore, LDLQR@NU-1000 could slow down the elevated blood sugar caused by maltose in mice and the area under blood sugar curve decreased by almost 20% when compared with the control group. The inflammatory factor (IL-1 beta , IL-6) in vivo and cell growth in vitro were almost the same between NU-1000 treatment and normal control groups. This study indicates NU-1000 is a promising vehicle for targeted peptide-based bioactive delivery to the small intestine.
引用
收藏
页码:55447 / 55457
页数:11
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