| Literature DB >> 32259072 |
Jihong Li1, Yoshiyuki Fukase2, Yi Shang3, Wei Zou4, José M Muñoz-Félix5, Lorena Buitrago1, Johannes van Agthoven6, Yixiao Zhang7, Ryoma Hara2, Yuta Tanaka2, Rei Okamoto2, Takeshi Yasui2, Takashi Nakahata2, Toshihiro Imaeda2, Kazuyoshi Aso2, Yuchen Zhou3, Charles Locuson8, Dragana Nesic1, Mark Duggan9, Junichi Takagi10, Roger D Vaughan11, Thomas Walz7, Kairbaan Hodivala-Dilke5, Steven L Teitelbaum4, M Amin Arnaout6, Marta Filizola3, Michael A Foley2, Barry S Coller1.
Abstract
The integrin αVβ3 receptor has been implicated in several important diseases, but no antagonists are approved for human therapy. One possible limitation of current small-molecule antagonists is their ability to induce a major conformational change in the receptor that induces it to adopt a high-affinity ligand-binding state. In response, we used structural inferences from a pure peptide antagonist to design the small-molecule pure antagonists TDI-4161 and TDI-3761. Both compounds inhibit αVβ3-mediated cell adhesion to αVβ3 ligands, but do not induce the conformational change as judged by antibody binding, electron microscopy, X-ray crystallography, and receptor priming studies. Both compounds demonstrated the favorable property of inhibiting bone resorption in vitro, supporting potential value in treating osteoporosis. Neither, however, had the unfavorable property of the αVβ3 antagonist cilengitide of paradoxically enhancing aortic sprout angiogenesis at concentrations below its IC50, which correlates with cilengitide's enhancement of tumor growth in vivo.Entities:
Year: 2019 PMID: 32259072 PMCID: PMC7088984 DOI: 10.1021/acsptsci.9b00041
Source DB: PubMed Journal: ACS Pharmacol Transl Sci ISSN: 2575-9108