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  • Amino acid conjugates of lithocholic acid as antagonists of the EphA2 receptor.

Amino acid conjugates of lithocholic acid as antagonists of the EphA2 receptor.

Journal of medicinal chemistry (2013-03-16)
Matteo Incerti, Massimiliano Tognolini, Simonetta Russo, Daniele Pala, Carmine Giorgio, Iftiin Hassan-Mohamed, Roberta Noberini, Elena B Pasquale, Paola Vicini, Silvia Piersanti, Silvia Rivara, Elisabetta Barocelli, Marco Mor, Alessio Lodola
摘要

The Eph receptor-ephrin system is an emerging target for the development of novel antiangiogenetic agents. We recently identified lithocholic acid (LCA) as a small molecule able to block EphA2-dependent signals in cancer cells, suggesting that its (5β)-cholan-24-oic acid scaffold can be used as a template to design a new generation of improved EphA2 antagonists. Here, we report the design and synthesis of an extended set of LCA derivatives obtained by conjugation of its carboxyl group with different α-amino acids. Structure-activity relationships indicate that the presence of a lipophilic amino acid side chain is fundamental to achieve good potencies. The l-Trp derivative (20, PCM126) was the most potent antagonist of the series disrupting EphA2-ephrinA1 interaction and blocking EphA2 phosphorylation in prostate cancer cells at low μM concentrations, thus being significantly more potent than LCA. Compound 20 is among the most potent small-molecule antagonists of the EphA2 receptor.

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Sigma-Aldrich
石胆酸, ≥95%
Sigma-Aldrich
链霉亲和素-过氧化物酶 来源于阿维丁链霉菌, lyophilized powder
石胆酸, European Pharmacopoeia (EP) Reference Standard