A dimeric bicyclic RGD ligand displays enhanced integrin binding affinity and strong biological effects on U-373 MG glioblastoma cells

Giovanni Sacco,Alberto Dal Corso,Daniela Arosio,Laura Belvisi,Mayra Paolillo,Luca Pignataro,Cesare Gennari

A dimeric bicyclic RGD ligand displays enhanced integrin binding affinity and strong biological effects on U-373 MG glioblastoma cells

2019

Giovanni Sacco
Alberto Dal Corso
Daniela Arosio
Laura Belvisi
Mayra Paolillo
Luca Pignataro
Cesare Gennari

A C2-symmetric bicyclic peptide bearing two RGD motifs was developed as a dimeric ligand, and it displayed enhanced inhibition of ECM protein binding to purified integrin receptors as compared to monomeric RGD analogues. Moreover, the dimeric bicyclic ligand induced cell detachment and inhibited FAK phosphorylation in U-373 MG glioblastoma cells.

Keywords:

Phosphorylation
Organic chemistry
Ligand (biochemistry)
Bicyclic molecule
Cell
Chemistry
Integrin
Ligand
Peptide
Biophysics
Receptor
Glioblastoma
Monomer
integrin binding

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