Steps toward mapping the human vasculature by phage display

Arap, Wadih; Kolonin, Mikhail G.; Trepel, Martin; Lahdenranta, Johanna; Cardó-Vila, Marina; Giordano, Ricardo J.; Mintz, Paul J.; Ardelt, Peter U.; Yao, Virginia J.; Vidal, Claudia I.; Chen, Limor; Flamm, Anne; Valtanen, Heli; Weavind, Lisa M.; Hicks, Marshall E.; Pollock, Raphael E.; Botz, Gregory H.; Bucana, Corazon D.; Koivunen, Erkki; Cahill, Dolores; Troncoso, Patricia; Baggerly, Keith A.; Pentz, Rebecca D.; Do, Kim-Anh; Logothetis, Christopher J.; Pasqualin, Renata

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Steps toward mapping the human vasculature by phage display

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Cahill, Dolores
Max Planck Society;

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Citation

Arap, W., Kolonin, M. G., Trepel, M., Lahdenranta, J., Cardó-Vila, M., Giordano, R. J., et al. (2002). Steps toward mapping the human vasculature by phage display. Nature Medicine, 8(2), 121-127.

Cite as: https://hdl.handle.net/11858/00-001M-0000-0010-8B7B-3

Abstract

The molecular diversity of receptors in human blood vessels remains largely unexplored. We developed a selection method in which peptides that home to specific vascular beds are identified after administration of a peptide library. Here we report the first in vivo screening of a peptide library in a patient. We surveyed 47,160 motifs that localized to different organs. This large-scale screening indicates that the tissue distribution of circulating peptides is nonrandom. High-throughput analysis of the motifs revealed similarities to ligands for differentially expressed cell-surface proteins, and a candidate ligand–receptor pair was validated. These data represent a step toward the construction of a molecular map of human vasculature and may have broad implications for the development of targeted therapies.