Solid-Phase Synthesis of a Nonpeptide RGD Mimetic Library:  New Selective αvβ3 Integrin Antagonists

The solid-phase synthesis of a low molecular weight RGD mimetic library is described. Activities of the compounds in inhibiting the interaction of ligands, vitronectin and fibrinogen, with isolated immobilized integrins αvβ3 and αIIbβ3 were determined in a screening assay. Highly active and selectiv...

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Published inJournal of medicinal chemistry Vol. 44; no. 12; pp. 1938 - 1950
Main Authors Sulyok, Gábor A. G, Gibson, Christoph, Goodman, Simon L, Hölzemann, Günter, Wiesner, Matthias, Kessler, Horst
Format Journal Article
LanguageEnglish
Published Washington, DC American Chemical Society 07.06.2001
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Abstract The solid-phase synthesis of a low molecular weight RGD mimetic library is described. Activities of the compounds in inhibiting the interaction of ligands, vitronectin and fibrinogen, with isolated immobilized integrins αvβ3 and αIIbβ3 were determined in a screening assay. Highly active and selective nonpeptide αvβ3 integrin antagonists with regard to orally bioavailability were developed, based on the aza-glycine containing lead compound 1. An important variation is the substitution of the aspartic amide of 1 by an aromatic residue. Furthermore, different guanidine mimetics have been incorporated to improve the pharmacokinetic profile. Exchange of the β-amino acid NH by a methylene moiety in one set of RGD mimetics leads to the azacarba analogue compounds representing a novel peptidomimetic approach, which should increase the metabolic stability.
AbstractList The solid-phase synthesis of a low molecular weight RGD mimetic library is described. Activities of the compounds in inhibiting the interaction of ligands, vitronectin and fibrinogen, with isolated immobilized integrins αvβ3 and αIIbβ3 were determined in a screening assay. Highly active and selective nonpeptide αvβ3 integrin antagonists with regard to orally bioavailability were developed, based on the aza-glycine containing lead compound 1. An important variation is the substitution of the aspartic amide of 1 by an aromatic residue. Furthermore, different guanidine mimetics have been incorporated to improve the pharmacokinetic profile. Exchange of the β-amino acid NH by a methylene moiety in one set of RGD mimetics leads to the azacarba analogue compounds representing a novel peptidomimetic approach, which should increase the metabolic stability.
Author Gibson, Christoph
Goodman, Simon L
Wiesner, Matthias
Hölzemann, Günter
Sulyok, Gábor A. G
Kessler, Horst
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Issue 12
Keywords Organic carbazate
Glycoprotein
Combinatorial chemistry
Non peptide compound
Vitronectin
Guanidines
Selectivity
In vitro
Integrin
Structure activity relation
Carboxylic acid
Chlorine Organic compounds
Chemical compound library
Benzenic compound
Antagonist
Solid phase
Chemical synthesis
Language English
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PublicationYear 2001
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Snippet The solid-phase synthesis of a low molecular weight RGD mimetic library is described. Activities of the compounds in inhibiting the interaction of ligands,...
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SubjectTerms Biological and medical sciences
Medical sciences
Miscellaneous
Pharmacology. Drug treatments
Title Solid-Phase Synthesis of a Nonpeptide RGD Mimetic Library:  New Selective αvβ3 Integrin Antagonists
URI http://dx.doi.org/10.1021/jm0004953
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