Journal article
Ibrutinib inhibits collagen-mediated but not ADP-mediated platelet aggregation
S Kamel, L Horton, L Ysebaert, M Levade, K Burbury, S Tan, M Cole-Sinclair, J Reynolds, R Filshie, S Schischka, A Khot, S Sandhu, MJ Keating, H Nandurkar, CS Tam
Leukemia | Published : 2014
DOI: 10.1038/leu.2014.247
Abstract
The BTK (Bruton's tyrosine kinase) inhibitor ibrutinib is associated with an increased risk of bleeding. A previous study reported defects in collagen- and adenosine diphosphate (ADP)-dependent platelet responses when ibrutinib was added ex vivo to patient samples. Whereas the collagen defect is expected given the central role of BTK in glycoprotein VI signaling, the ADP defect lacks a mechanistic explanation. In order to determine the real-life consequences of BTK platelet blockade, we performed light transmission aggregometry in 23 patients receiving ibrutinib treatment. All patients had reductions in collagen-mediated platelet aggregation, with a significant association between the degree..
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Awarded by National Institutes of Health