Identification of the first enantiopure Rac1-Tiam1 protein-protein interaction inhibitor and its optimized synthesis via phosphine free remote group directed hydroarylation

Alessandro Ruffoni; Nicola Ferri; Andrea Pinto; Sara Pellegrino; Alessandro Contini; Francesca Clerici

doi:10.1039/c8md00477c

Identification of the first enantiopure Rac1-Tiam1 protein-protein interaction inhibitor and its optimized synthesis via phosphine free remote group directed hydroarylation

Medchemcomm. 2018 Dec 26;10(2):310-314. doi: 10.1039/c8md00477c. eCollection 2019 Feb 1.

Authors

Alessandro Ruffoni¹, Nicola Ferri², Andrea Pinto³, Sara Pellegrino⁴, Alessandro Contini⁴, Francesca Clerici⁴

Affiliations

¹ School of Chemistry , University of Manchester , Manchester , M13 9PL , UK . Email: [email protected].
² Department of Pharmaceutical and Pharmacological Sciences , Via Marzolo 5 , 35131 Padua , Italy.
³ Department of Food, Environmental and Nutritional Sciences (DeFENS) , Via Mangiagalli 25 , 20133 Milano , Italy.
⁴ Department of Pharmaceutical Sciences , General and Organic Chemistry Section "Alessandro Marchesini" , Via Venezian 21 , 20133 Milano , Italy . Email: [email protected].

Abstract

A phospine free hydroarylation reaction applied to norbornene derivatives is described for the first time and was exploited for the regioselective gram scale synthesis of AR-148, a known Rac1-Tiam1 PPI inhibitor. Umpolung conversion of the nitro group into free amine allowed the regiocontrol of the key arylation step via a long range effect. The effect of AR-148 in comparison with its enantiomers on Rac1 activation of has been evaluated and (-)AR-148 has been identified as the first enantiomerically pure inhibitor of Rac1-Tiam1 PPI.