Samantha Deianira Dattoli scite author profile

A novel series of β-lactam derivatives that was designed and synthesized to target RGD-binding and leukocyte integrins is reported. The compound library was evaluated by investigating the effects on integrin-mediated cell adhesion and cell signaling in cell lines expressing αβ, αβ, αβ, αβ, αβ, αβ, and αβ integrins. SAR analysis of the new series of azetidinones enabled the recognition of structural elements associated with integrin selectivity. We obtained selective and potent agonists that could induce cell adhesion and promote cell signaling mediated by αβ, αβ, αβ, or αβ integrin, and antagonists for the integrins αβ and αβ as well as αβ and αβ, preventing the effects elicited by the respective endogenous agonists.

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Targeting integrins αvβ3 and α5β1 with new β-lactam derivatives

Galletti

Soldati

Pori

et al. 2014

European Journal of Medicinal Chemistry

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DS‐70, a novel and potent α₄ integrin antagonist, is an effective treatment for experimental allergic conjunctivitis in guinea pigs

Dattoli

Baiula

Marco

et al. 2018

British J Pharmacology

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Dehydro-β-proline Containing α₄β₁ Integrin Antagonists: Stereochemical Recognition in Ligand–Receptor Interplay

Tolomelli

Baiula

Viola

et al. 2015

ACS Med. Chem. Lett.

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A novel class of dehydro-β-proline-containing peptidomimetics, designed to be effective as α4β1 integrin ligands, has been developed on the basis of the fundamental requirements for the interactions of these transmembrane receptors with bioactive ligands. Dehydro-β-proline ring has been synthesized through an original pathway, involving ring closing metathesis of a diallylamino derivative. The synthesized products showed to be effective and selective as α4β1 integrin antagonists and displayed IC50 values in the nanomolar range in cell adhesion inhibition assays and in VCAM-1-induced phosphorylation of extracellular-signal-regulated kinases. Significant activity was observed also toward the homologous integrin α4β7, while they did not display any activity toward selected members of β1, β2, and β3 families. A strong dependence on the stereochemistry of the heterocyclic central core could be observed. The great importance of α4β1 integrin in chronic inflammatory and autoimmune diseases suggests a possible exploitation of these ligands as lead compounds for therapeutic tools development.

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Modulation of αvβ3- and α5β1-integrin-mediated adhesion by dehydro-β-amino acids containing peptidomimetics

Tolomelli

Baiula

Belvisi

et al. 2013

European Journal of Medicinal Chemistry

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