Biotin receptor-mediated intracellular delivery of synthetic polypeptide-protein complexes

被引:12
作者
Li, H. [1 ]
Bruce, G. [1 ]
Childerhouse, N. [2 ]
Keegan, G. [2 ]
Mantovani, G. [1 ]
Stolnik, S. [1 ]
机构
[1] Univ Nottingham, Sch Pharm, Mol Therapeut & Formulat Div, Nottingham, England
[2] Vectura Grp Plc, Chippenham, England
关键词
Intracellular protein delivery; Polymer complexes; Biotin targeting; Endocytosis; Lung delivery; PANTOTHENIC-ACID; CHOLESTEROL; ENDOCYTOSIS; TRANSPORT; CAVEOLAE; NANOPARTICLES; INTERNALIZATION; TRANSCYTOSIS; MECHANISMS; EXPRESSION;
D O I
10.1016/j.jconrel.2023.03.051
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Pulmonary delivery offers a non-invasive route for the administration of biotherapeutics. In this context, understanding and control of a transport into, and across cellular barriers is central to the design of delivery systems. Here, we report our study on receptor mediated delivery of protein cargo by a formulation comprising sub300 nm sized non-covalent protein complexes with biotin-conjugated PEG-poly(glutamic acid) (biotin-PEG2k-bGA10) and PEG2k-b-GA30 copolymers blend as targeting and complexing functionalities. Designed complexes achieve intracellular delivery of the cargo in lung derived A549 epithelial cells in vitro via sodium-dependent multivitamin transporter (biotin receptor). We further show that biotin receptor driven endocytosis preferentially involves dynamin- and caveolae-dependent vesicular internalization, switching the transport pathway away from predominantly clathrin-dependent entry of free protein. Significantly for a protective intracellular delivery of biotherapeutics based on non-covalent complexation with polymeric excipients, the study provides evidence of intracellular presence of the complexing copolymer; demonstrated exploiting biotin in biotin-PEG2kb-GA10 copolymer as a tag for binding with fluorescently labelled avidin. Moreover, analysis of intracellular localization of constitutive species shortly following cellular internalization suggests a co-localization of biotinPEG2k-b-GA10 copolymer and protein constitutive species. The study demonstrates intracellular delivery of biotin targeted non-covalent complexes with a protein cargo, the result with important implications in a design of enabling technology platforms for protective, receptor mediated intracellular delivery of biotherapeutics.
引用
收藏
页码:333 / 341
页数:9
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