Nonclinical Antiangiogenesis and Antitumor Activities of Axitinib (AG-013736), an Oral, Potent, and Selective Inhibitor of Vascular Endothelial Growth Factor Receptor Tyrosine Kinases 1, 2, 3

Abstract: Purpose: Axitinib (AG-013736) is a potent and selective inhibitor of vascular endothelial growth factor (VEGF) receptor tyrosine kinases 1to 3 that is in clinical development for the treatment of solid tumors. We provide a comprehensive description of its in vitro characteristics and activities, in vivo antiangiogenesis, and antitumor efficacy and translational pharmacology data. Experimental Design: The potency, kinase selectivity, pharmacologic activity, and antitumor efficacy of axitinib were assessed in va… Show more

“…Axitinib is more selective and principally inhibits VEGFR1-3, PDGFRs and KIT [41]. Axitinib has shown benefit in renal cell carcinoma, and is currently under study in a national phase II clinical trial for advanced soft tissue sarcoma.…”

“…A screening array of 242 kinases showed 0.3µmol/l sunitinib inhibited the activity of 49 kinases by more than 50% including VEGFR1-3, PDGFRs, KIT, FLT3, CSF-1R and RET [187]. Axitinib is more selective, principally inhibiting VEGFR1-3, PDGFR and KIT (table 4.1) [41]. At doses above 1µmol/l however axitinib also inhibits Abl, Aurora B, Arg, AMPK, Axl and MST2 [41].…”

“…Axitinib is more selective, principally inhibiting VEGFR1-3, PDGFR and KIT (table 4.1) [41]. At doses above 1µmol/l however axitinib also inhibits Abl, Aurora B, Arg, AMPK, Axl and MST2 [41]. In vitro, axitinib reduced HUVEC survival and inhibited tubule formation by HuDMEC spheroids [41].…”

“…At doses above 1µmol/l however axitinib also inhibits Abl, Aurora B, Arg, AMPK, Axl and MST2 [41]. In vitro, axitinib reduced HUVEC survival and inhibited tubule formation by HuDMEC spheroids [41]. Axitinib is currently under study in a phase II clinical trial for advanced soft tissue sarcoma, …”

“…Axitinib inhibits FGFR1 phosphorylation, with an IC 50 of 215nmol/l (i.e. 83ng/ml) [41]. Minor responses were seen to axitinib at doses up to 250ng/ml in functional assays of ASM and ISO-HAS cells, suggesting co-inhibition of VEGF and FGF signalling was not beneficial.…”

Vascular-targeted agents for the treatment of angiosarcoma

“…Axitinib is more selective and principally inhibits VEGFR1-3, PDGFRs and KIT [41]. Axitinib has shown benefit in renal cell carcinoma, and is currently under study in a national phase II clinical trial for advanced soft tissue sarcoma.…”

“…A screening array of 242 kinases showed 0.3µmol/l sunitinib inhibited the activity of 49 kinases by more than 50% including VEGFR1-3, PDGFRs, KIT, FLT3, CSF-1R and RET [187]. Axitinib is more selective, principally inhibiting VEGFR1-3, PDGFR and KIT (table 4.1) [41]. At doses above 1µmol/l however axitinib also inhibits Abl, Aurora B, Arg, AMPK, Axl and MST2 [41].…”

“…Axitinib is more selective, principally inhibiting VEGFR1-3, PDGFR and KIT (table 4.1) [41]. At doses above 1µmol/l however axitinib also inhibits Abl, Aurora B, Arg, AMPK, Axl and MST2 [41]. In vitro, axitinib reduced HUVEC survival and inhibited tubule formation by HuDMEC spheroids [41].…”

“…At doses above 1µmol/l however axitinib also inhibits Abl, Aurora B, Arg, AMPK, Axl and MST2 [41]. In vitro, axitinib reduced HUVEC survival and inhibited tubule formation by HuDMEC spheroids [41]. Axitinib is currently under study in a phase II clinical trial for advanced soft tissue sarcoma, …”

“…Axitinib inhibits FGFR1 phosphorylation, with an IC 50 of 215nmol/l (i.e. 83ng/ml) [41]. Minor responses were seen to axitinib at doses up to 250ng/ml in functional assays of ASM and ISO-HAS cells, suggesting co-inhibition of VEGF and FGF signalling was not beneficial.…”

Vascular-targeted agents for the treatment of angiosarcoma

Structure‐Based Design and Characterization of Axitinib

VEGFR/Multikinase Inhibitors