Enhanced oral and pulmonary delivery of biomacromolecules via amplified transporter targeting

福斯科林 并行传输 纳米载体 药理学 丁酸盐 跨细胞 细胞内 顶膜 化学 细胞 医学 内吞作用 受体 生物化学 药品 磁导率 发酵
作者
Xin Xiao,Lie Zhang,Mingjie Ni,Xi Liu,Liyun Xing,Licheng Wu,Zhou Zhou,Lian Li,Jingyuan Wen,Yuan Huang
出处
期刊:Journal of Controlled Release [Elsevier BV]
卷期号:370: 152-167 被引量:10
标识
DOI:10.1016/j.jconrel.2024.04.026
摘要

Ligand-modified nanocarriers can promote oral or inhalative administration of macromolecular drugs across the intestinal or pulmonary mucosa. However, enhancing the unidirectional transport of the nanocarriers through "apical uptake→intracellular transport→basolateral exocytosis" route remains a hot topic and challenge in current research. Forskolin is a naturally occurring diterpenoid compound extracted from the roots of C. forskohlii. In our studies, we found that forskolin could increase the transcellular transport of butyrate-modified nanoparticles by 1.67-fold and 1.20-fold in Caco-2 intestinal epithelial cell models and Calu-3 lung epithelial cell models, respectively. Further mechanistic studies revealed that forskolin, on the one hand, promoted the cellular uptake of butyrate-modified nanoparticles by upregulating the expression of monocarboxylic acid transporter-1 (MCT-1) on the apical membrane. On the other hand, forskolin facilitated the binding of MCT-1 to caveolae, thereby mediating butyrate-modified nanoparticles hijacking caveolae to promote the basolateral exocytosis of butyrate-modified nanoparticles. Studies in normal mice model showed that forskolin could promote the transmucosal absorption of butyrate-modified nanoparticles by >2-fold, regardless of oral or inhalative administration. Using semaglutide as the model drug, both oral and inhalation delivery approaches demonstrated significant hypoglycemic effects in type 2 diabetes mice model, in which inhalative administration was more effective than oral administration. This study optimized the strategies aimed at enhancing the transmucosal absorption of ligand-modified nanocarriers in the intestinal or pulmonary mucosa.
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