Straightforward synthesis of bis-tetraazacycloalkanes: towards new potential CXCR4 antagonists?

Nicolas Sok; Isabelle Baglin; Christelle Basset; Fatima Fakkor; Evelyne Kohli; Yoann Rousselin; Claire Bernhard; Frédéric Boschetti; Christine Goze; Franck Denat

doi:10.1039/C7RA04218C

Straightforward synthesis of bis-tetraazacycloalkanes: towards new potential CXCR4 antagonists?†

Nicolas Sok,

*^a Isabelle Baglin,^b Christelle Basset,^c Fatima Fakkor,^d Evelyne Kohli,^c Yoann Rousselin,^b Claire Bernhard,^b Frédéric Boschetti,^e Christine Goze^b and Franck Denat*^b

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* Corresponding authors

^a Univ. Bourgogne Franche-Comté, AgroSup Dijon, PAM UMR A 02.102, F-21000 Dijon, France
E-mail: nicolas.sok@agrosupdijon.fr

^b Institut de Chimie Moléculaire de l'Université de Bourgogne, UMR CNRS 6302, Univ. Bourgogne Franche-Comté, 9 Avenue Alain Savary, 21078 Dijon Cedex, France
E-mail: franck.denat@u-bourgogne.fr

^c INSERM UMR 866, UFR des Sciences de Santé, Univ. Bourgogne Franche-Comté, Dijon, France

^d Centre Hospitalier Universitaire, Dijon, France

^e Chematech S.A., 2 Rue Pauline Kergomard, 21000 Dijon, France

Abstract

We report herein an efficient and general method for the synthesis of new bismacrocyclic compounds, structural analogues of biscyclam AMD3100, in which the two macrocycles are linked together through carbon atoms of the cycles. Several representatives of this new class of biscyclic derivatives were prepared by reacting C-aminomethyl-13aneN4 with aromatic dialdehydes. Preliminary in vitro studies were performed to evaluate the affinity of these compounds towards the co-receptor CXCR4.

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Straightforward synthesis of bis-tetraazacycloalkanes: towards new potential CXCR4 antagonists?†

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Straightforward synthesis of bis-tetraazacycloalkanes: towards new potential CXCR4 antagonists?

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