Development of an orally-administrable tumor vasculature-targeting therapeutic using annexin A1-binding D-peptides

Author:

Nonaka Motohiro,Mabashi-Asazuma Hideaki,Jarvis Donald L.,Yamasaki Kazuhiko,Akama Tomoya O.,Nagaoka Masato,Sasai Toshio,Kimura-Takagi Itsuko,Suwa Yoichi,Yaegashi Takashi,Huang Chun-Teng,Nishizawa-Harada Chizuko,Fukuda Michiko N.ORCID

Abstract

We previously reported that IF7 peptide, which binds to the annexin A1 (ANXA1) N-terminus, functions as a tumor vasculature-targeted drug delivery vehicle after intravenous injection. To enhance IF7 stability in vivo, we undertook mirror-image peptide phage display using a synthetic D-peptide representing the ANXA1 N-terminus as target. We then identified peptide sequences, synthesized them as D-amino acids, and designated the resulting peptide dTIT7, which we showed bound to the ANXA1 N-terminus. Whole body imaging of mouse brain tumor models injected with near infrared fluorescent IRDye-conjugated dTIT7 showed fluorescent signals in brain and kidney. Furthermore, orally-administered dTIT7/geldanamycin (GA) conjugates suppressed brain tumor growth. Ours is a proof-of-concept experiment showing that ANXA1-binding D-peptide can be developed as an orally-administrable tumor vasculature-targeted therapeutic.

Funder

National Institutes of Health

Japan Agency for Medical Research and Development

Nakajima Foundation

Publisher

Public Library of Science (PLoS)

Subject

Multidisciplinary

Reference36 articles.

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