Abstract 2620: 3D multicellular pancreatic cancer spheroids as drug screening tool for pharmacological evaluation of EHT 5372 and other Mirk/DYRK1B inhibitors

Abstract: The dual-specificity tyrosine phosphorylated and regulated kinase Mirk/DYRK1B belongs to an evolutionary conserved family of kinases involved in the control of growth and development. DYRK1B has low level of expression in most normal cell types but is amplified or over-expressed in a number of human cancers. DYRK1B regulates the exit of cancer cells from quiescence through regulating cyclin D turnover and p27kip1 stabilization, thus participating as substantial actor in the control of cancer cell cycle progres… Show more

“…These results suggested that both compounds not only exhibited high potency in vitro but demonstrated also good activities in cell-based systems and in vivo models. These data therefore suggest a potential use of this class of inhibitors for targeting cancer cells with high DYRK1A/1B kinase activities. − …”

“…Inhibitor 1 compared favorably to harmine, leucettine L41, and to the reactive and promiscuous compound epigallo-catechin-gallate EGCG In addition, it normalized Aβ-induced Tau phosphorylation in neuronal cells and also normalized DYRK1A-induced Aβ production in APP overexpressing cells . In addition, in vitro characterization in various cancer cellular models showed that the inhibitor targeted G0/G1 transition and reduced stemness and EMT properties of cancer cells organized in spheroids . Furthermore, it demonstrated promising activities in patient-derived ovarian cancer ascites spheroids and in vivo activities in a Panc1 xenograft model without detectable toxicity in mice .…”

An Unusual Binding Model of the Methyl 9-Anilinothiazolo[5,4-f] quinazoline-2-carbimidates (EHT 1610 and EHT 5372) Confers High Selectivity for Dual-Specificity Tyrosine Phosphorylation-Regulated Kinases

“…These results suggested that both compounds not only exhibited high potency in vitro but demonstrated also good activities in cell-based systems and in vivo models. These data therefore suggest a potential use of this class of inhibitors for targeting cancer cells with high DYRK1A/1B kinase activities. − …”

“…Inhibitor 1 compared favorably to harmine, leucettine L41, and to the reactive and promiscuous compound epigallo-catechin-gallate EGCG In addition, it normalized Aβ-induced Tau phosphorylation in neuronal cells and also normalized DYRK1A-induced Aβ production in APP overexpressing cells . In addition, in vitro characterization in various cancer cellular models showed that the inhibitor targeted G0/G1 transition and reduced stemness and EMT properties of cancer cells organized in spheroids . Furthermore, it demonstrated promising activities in patient-derived ovarian cancer ascites spheroids and in vivo activities in a Panc1 xenograft model without detectable toxicity in mice .…”

An Unusual Binding Model of the Methyl 9-Anilinothiazolo[5,4-f] quinazoline-2-carbimidates (EHT 1610 and EHT 5372) Confers High Selectivity for Dual-Specificity Tyrosine Phosphorylation-Regulated Kinases