Since mutations of Ras genes have a great incidence in human tumours, Ras oncoproteins are a major clinical target for the development of anticancer agents. We have developed synthetic molecules able to inhibit Ras activation. Here we present new, water-soluble Ras inhibitors composed by an aromatic pharmacofore moiety covalently linked to different sugars. New glycosylated compounds bind to Switch 2 region of Ras, also involved in effector binding, inhibit GEF-catalyzed nucleotide exchange on Ras in vitro, and reduce Ras-dependent proliferation of murine fibroblasts. The influence of the sugar unit on Ras binding affinity and on the biological activity of Ras inhibitors has been investigated.
Sacco, E., Abraham, S., Palmioli, A., Damore, G., Bargna, A., Mazzoleni, E., et al. (2011). Binding properties and biological characterization of new sugar-derived Ras ligands. MEDCHEMCOMM, 2(5), 396-401 [10.1039/C0MD00264J].
Binding properties and biological characterization of new sugar-derived Ras ligands
SACCO, ELENA;PALMIOLI, ALESSANDRO;MAZZOLENI, ELISA;VANONI, MARCO ERCOLE;PERI, FRANCESCO
2011
Abstract
Since mutations of Ras genes have a great incidence in human tumours, Ras oncoproteins are a major clinical target for the development of anticancer agents. We have developed synthetic molecules able to inhibit Ras activation. Here we present new, water-soluble Ras inhibitors composed by an aromatic pharmacofore moiety covalently linked to different sugars. New glycosylated compounds bind to Switch 2 region of Ras, also involved in effector binding, inhibit GEF-catalyzed nucleotide exchange on Ras in vitro, and reduce Ras-dependent proliferation of murine fibroblasts. The influence of the sugar unit on Ras binding affinity and on the biological activity of Ras inhibitors has been investigated.
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