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International Journal of Molecular Sciences 2020-Sep

Ponatinib and other CML Tyrosine Kinase Inhibitors in Thrombosis

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Peng Zeng
Alvin Schmaier

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Abstrakt

Abl1 kinase has important biological roles. The Bcr-Abl1 fusion protein creates undesired kinase activity and is pathogenic in 95% of chronic myeloid leukemia (CML) and 30% of acute lymphoblastic leukemia (ALL) patients. Targeted therapies to these diseases are tyrosine kinase inhibitors. The extent of a tyrosine kinase inhibitor's targets determines the degree of biologic effects of the agent that may influence the well-being of the patient. This fact is especially true with tyrosine kinase inhibitor effects on the cardiovascular system. Thirty-one percent of ponatinib-treated patients, the tyrosine kinase inhibitor with the broadest inhibitory spectrum, have thrombosis associated with its use. Recent experimental investigations have indicated the mechanisms of ponatinib-associated thrombosis. Further, an antidote to ponatinib is in development by re-purposing an FDA-approved medication.

Keywords: Abl1 kinase; Bcr-Abl1; chronic myelogenous leukemia; pioglitazone; platelet hyperactivity; ponatinib; thrombosis; tyrosine kinase inhibitors.

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