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Neutral 5-substituted 4-indazolylaminoquinazolines as potent, orally active inhibitors of erbB2 receptor tyrosine kinase
Authors:Barlaam Bernard  Acton David G  Ballard Peter  Bradbury Robert H  Cross Darren  Ducray Richard  Germain Hervé  Hudson Kevin  Klinowska Teresa  Magnien Françoise  Ogilvie Donald J  Olivier Annie  Ross Helen S  Smith Robin  Trigwell Cath B  Vautier Michel  Wright Lindsay
Institution:AstraZeneca, Centre de Recherches, Z.I.S.E. La Pompelle, B.P. 1050, 51689 Reims Cedex 2, France. bernard.barlaam2@astrazeneca.com
Abstract:We have identified a new series of C-5 substituted indazolylaminoquinazolines as potent erbB2 kinase inhibitors. The lead compound 22 showed excellent in vitro potency, good physical properties, acceptable oral pharmacokinetics in rat and dog, and low human in vitro clearance. It showed at least equivalent activity dose for dose compared to lapatinib in various erbB2- or EGFR-driven xenograft models after chronic oral administration.
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