Targeted drug delivery via caveolae-associated protein PV1 improves lung fibrosis

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作者
Gabriela M. Marchetti
Timothy J. Burwell
Norman C. Peterson
Jennifer A. Cann
Richard N. Hanna
Qing Li
Emily L. Ongstad
Jonathan T. Boyd
Maureen A. Kennedy
Weiguang Zhao
Keith W. Rickert
Joseph S. Grimsby
William F. Dall’Acqua
Herren Wu
Ping Tsui
M. Jack Borrok
Ruchi Gupta
机构
[1] MedImmune,Antibody Discovery & Protein Engineering
[2] MedImmune,Cardiovascular & Metabolic Diseases
[3] MedImmune,Respiratory, Inflammation and Autoimmune Diseases
[4] MedImmune,Translational Sciences
[5] MedImmune,Pathology
[6] MedImmune,Microbial Sciences
来源
Communications Biology | / 2卷
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摘要
Systemic administration of bio-therapeutics can result in only a fraction of drug reaching targeted tissues, with the majority of drug being distributed to tissues irrelevant to the drug’s site of action. Targeted delivery to specific organs may allow for greater accumulation, better efficacy, and improved safety. We investigated how targeting plasmalemma vesicle-associated protein (PV1), a protein found in the endothelial caveolae of lungs and kidneys, can promote accumulation in these organs. Using ex vivo fluorescence imaging, we show that intravenously administered αPV1 antibodies localize to mouse lungs and kidneys. In a bleomycin-induced idiopathic pulmonary fibrosis (IPF) mouse model, αPV1 conjugated to Prostaglandin E2 (PGE2), a known anti-fibrotic agent, significantly reduced collagen content and fibrosis whereas a non-targeted PGE2 antibody conjugate failed to slow fibrosis progression. Our results demonstrate that PV1 targeting can be utilized to deliver therapeutics to lungs and this approach is potentially applicable for various lung diseases.
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