2017
DOI: 10.1182/bloodadvances.2017011999
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Severe platelet dysfunction in NHL patients receiving ibrutinib is absent in patients receiving acalabrutinib

Abstract: The Bruton tyrosine kinase (Btk) inhibitor ibrutinib induces platelet dysfunction and causes increased risk of bleeding. Off-target inhibition of Tec is believed to contribute to platelet dysfunction and other side effects of ibrutinib. The second-generation Btk inhibitor acalabrutinib was developed with improved specificity for Btk over Tec. We investigated platelet function in patients with non-Hodgkin lymphoma (NHL) receiving ibrutinib or acalabrutinib by aggregometry and by measuring thrombus formation on … Show more

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Cited by 103 publications
(142 citation statements)
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“…27 Inhibition of other kinases than BTK has been suggested to be involved in some of these adverse effects, such as inhibitory effect on platelet function. 28 Based on our present results, the concomitant use of currently available 70-mg and 140-mg capsules of ibrutinib with itraconazole or other strong CYP3A4 inhibitors increases ibrutinib exposure to a higher level than what is observed when the usual 420-mg or 560-mg daily doses are taken without CYP3A4 inhibitors. Such a high exposure could increase the risk of concentration-dependent adverse effects and lead to discontinuation of the treatment and potentially affect clinical outcomes.…”
Section: Itraconazole Increases Ibrutinib Exposuresupporting
confidence: 56%
“…27 Inhibition of other kinases than BTK has been suggested to be involved in some of these adverse effects, such as inhibitory effect on platelet function. 28 Based on our present results, the concomitant use of currently available 70-mg and 140-mg capsules of ibrutinib with itraconazole or other strong CYP3A4 inhibitors increases ibrutinib exposure to a higher level than what is observed when the usual 420-mg or 560-mg daily doses are taken without CYP3A4 inhibitors. Such a high exposure could increase the risk of concentration-dependent adverse effects and lead to discontinuation of the treatment and potentially affect clinical outcomes.…”
Section: Itraconazole Increases Ibrutinib Exposuresupporting
confidence: 56%
“…Although clinical data were still being accumulated, an earlier hypothesis based on kinase affinity data proposed that acalabrutinib might lead to lower bleeding rates because of its higher selectivity for BTK relative to TEC (Byrd et al, 2016;Barf et al, 2017;Awan et al, 2019). However, when properly adjusted for clinical exposure, covalent binding mechanism, and enzymatic activity, our data and those of other groups (Bye et al, 2017) now indicate that ibrutinib and acalabrutinib have similar selectivity between BTK and TEC. This similar selectivity is consistent with a recent study suggesting that platelet inhibition and potential hemorrhagic risk predicted by in vitro closure time are likelyclass effects across five BTK inhibitors: ibrutinib, zanubrutinib, acalabrutinib, tirabrutinib, and evobrutinib (Denzinger et al, 2019).…”
Section: Discussionmentioning
confidence: 46%
“…Acalabrutinib is a covalent inhibitor of C481S in the ATP binding pocket of BTK with a short half‐life. Acalabrutinib and its major metabolite ACP‐5862 have limited off‐target kinase activity, inhibiting only two kinases [ErbB4] and the BMX gene in chromosome X. Acalabrutinib preserves Src family kinase (collagen to platelet adhesion) activity and thus avoids the unstable platelet thrombus formation seen with ibrutinib therapy . These mechanisms potentially explain why the risk of bleeding and atrial fibrillation is significantly more minimal with acalabrutinib compared to ibrutinib.…”
Section: Advances In the Treatment Of MCLmentioning
confidence: 99%