Targeted Phage Display-based Pulmonary Vaccination in Mice and Non-human Primates.

生物 病毒学 抗体 免疫学 免疫系统 噬菌体疗法
作者
Daniela I. Staquicini,E. Magda Barbu,Rachel L. Zemans,Beth K. Dray,Fernanda I. Staquicini,Prashant Dogra,Marina Cardó-Vila,Cindy K. Miranti,Wallace B. Baze,Luisa L. Villa,Jorge Kalil,Geetanjali Sharma,Eric R. Prossnitz,Zhihui Wang,Vittorio Cristini,Richard L. Sidman,Andrew Berman,Reynold A. Panettieri,Rubin M. Tuder,Renata Pasqualini,Wadih Arap
出处
期刊:Med [Elsevier]
卷期号:2 (3): 321-342 被引量:6
标识
DOI:10.1016/j.medj.2020.10.005
摘要

Summary Background The extensive alveolar capillary network of the lungs is an attractive route for the administration of several agents. One key functional attribute is the rapid onset of systemic action due to the absence of first-pass metabolism. Methods Here, we applied a combinatorial approach for ligand-directed pulmonary delivery as a unique route for systemic targeting in vaccination. Findings We screened a phage display random peptide library in vivo to select, identify, and validate a ligand (CAKSMGDIVC) that specifically targets and is internalized through its receptor, α3β1 integrin, on the surface of cells lining the lung airways and alveoli and mediates CAKSMGDIVC-displaying phage binding and systemic delivery without compromising lung homeostasis. As a proof-of-concept, we show that the pulmonary delivery of targeted CAKSMGDIVC-displaying phage particles in mice and non-human primates elicits a systemic and specific humoral response. Conclusions This broad methodology blueprint represents a robust and versatile platform tool enabling new ligand-receptor discovery with many potential translational applications. Funding Cancer Center Support Grants to the University of Texas M.D. Anderson Cancer Center ( CA016672 ), University of New Mexico Comprehensive Cancer Center ( CA118100 ), Rutgers Cancer Institute of New Jersey ( CA072720 ), research awards from the Gillson-Longenbaugh Foundation , and National Institutes of Health (NIH) grant no. 1R01CA226537 .

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