Structure-Function Study of Quinazolinone-Based Vitronectin Receptor (αVβ3) Antagonists: Computer-Assisted Analysis of Ligand-Receptor Interactions

Edward   C.   Lawson; William   A.   Kinney; Michael   J.   Costanzo; William   J.   Hoekstra; Jack   A.   Kauffman; Diane   K.   Luci; Rosemary      Santulli; Brett   A.   Tounge; Stephen   C.   Yabut; Patricia      Andrade-Gordon

Letters in Drug Design & Discovery

Author(s): Edward C. Lawson, William A. Kinney, Michael J. Costanzo, William J. Hoekstra, Jack A. Kauffman, Diane K. Luci, Rosemary Santulli, Brett A. Tounge, Stephen C. Yabut and Patricia Andrade-Gordon

DOI: 10.2174/1570180043485644

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Structure-Function Study of Quinazolinone-Based Vitronectin Receptor (αVβ3) Antagonists: Computer-Assisted Analysis of Ligand-Receptor Interactions

Page: [14 - 18] Pages: 5

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Abstract

Modification of the pendant functionalities on a quinazolinone scaffold led to potent antagonist activity for integrin αVβ3 with selectivity over integrin αIIbβ3. Various guanidine mimetics, linkers, and arylsulfonamides were investigated to optimize the series. A molecular model was constructed based on a published X-ray structure and used to analyze ligand-receptor interactions. We identified key interactions for the quinazolinone and arylsulfonamide groups that may explain the changes in potency in the structure-function study.

Keywords: Quinazolinone, Vitronectin Receptor, Ligand-Receptor

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