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用于增强鼻腔胰岛素递送的苯基硼酸修饰纳米平台的内化机制

Internalization Mechanism of Phenylboronic-Acid-Decorated Nanoplatform for Enhanced Nasal Insulin Delivery.

作者信息

Wei Xiaosong, Duan Xiaozhuang, Zhang Yufei, Ma Zhuang, Li Chaoxing, Zhang Xinge

机构信息

Key Laboratory of Functional Polymer Materials of Ministry of Education, Institute of Polymer Chemistry, College of Chemistry, Nankai University, Tianjin 300071, China.

出版信息

ACS Appl Bio Mater. 2020 Apr 20;3(4):2132-2139. doi: 10.1021/acsabm.0c00002. Epub 2020 Feb 20.

Abstract

Insulin injection causes great pain to the patient, and nasal mucosal administration of insulin is a novel route for the treatment of diabetes. This strategy could protect insulin from either extensive first-pass metabolism or enzyme degradation in the gastrointestinal tract. With the dynamic boronate esters reversibly formed by phenylboronic acid and diols on nasal mucosal epithelial cell surfaces, we herein developed phenylboronic-acid-functionalized dextran nanoplatforms to enhance the permeability of cargos and boost penetration. The nanoplatforms with excellent loading capacity exhibited significant endocytosis compared with naked insulin. The mechanism of endocytosis was involved in clathrin- and lipid raft/caveolae-dependent endocytic pathways. The in vivo nasal delivery of insulin suggested that these nanoplatforms did not trigger nasal epithelial inflammation and greatly decreased blood sugar levels and improved insulin bioavailability. Collectively, this proof-of-concept study demonstrates a novel carrier of phenylboronic-acid-decorated polymer for insulin delivery and provides a promising approach for the development of a diabetes therapeutic strategy.

摘要

胰岛素注射会给患者带来巨大痛苦,而胰岛素的鼻腔黏膜给药是一种治疗糖尿病的新途径。该策略可保护胰岛素免受广泛的首过代谢或胃肠道中的酶降解。利用苯基硼酸与二醇在鼻腔黏膜上皮细胞表面可逆形成的动态硼酸酯,我们在此开发了苯基硼酸功能化的葡聚糖纳米平台,以增强货物的通透性并促进渗透。与裸胰岛素相比,具有优异负载能力的纳米平台表现出显著的内吞作用。内吞作用机制涉及网格蛋白和脂筏/小窝依赖性内吞途径。胰岛素的体内鼻腔给药表明,这些纳米平台不会引发鼻上皮炎症,且能大幅降低血糖水平并提高胰岛素生物利用度。总的来说,这项概念验证研究证明了一种用于胰岛素递送的苯基硼酸修饰聚合物的新型载体,并为开发糖尿病治疗策略提供了一种有前景的方法。

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