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Journal article

Low-dose Btk inhibitors selectively block platelet activation by CLEC-2

Abstract:
Inhibitors of the tyrosine kinase Btk have been proposed as novel antiplatelet agents. In this study we show that low concentrations of the Btk inhibitor ibrutinib block CLEC-2-mediated activation and tyrosine phosphorylation including Syk and PLCγ2 in human platelets. Activation is also blocked in patients with X-linked agammaglobulinaemia (XLA) caused by a deficiency or absence of Btk. In contrast, the response to GPVI is delayed in the presence of low concentrations of ibrutinib or in patients with XLA, and tyrosine phosphorylation of Syk is preserved. A similar set of results is seen with the second-generation inhibitor, acalabrutinib. The differential effect of Btk inhibition in CLEC-2 relative to GPVI signalling is explained by the positive feedback role involving Btk itself, as well as ADP and thromboxane A2 mediated activation of P2Y12 and TP receptors, respectively. This feedback role is not seen in mouse platelets and, consistent with this, CLEC-2-mediated activation is blocked by high but not by low concentrations of ibrutinib. Nevertheless, thrombosis was absent in 8 out of 13 mice treated with ibrutinib. These results show that Btk inhibitors selectively block activation of human platelets by CLEC-2 relative to GPVI suggesting that they can be used at ‘low dose’ in patients to target CLEC-2 in thrombo-inflammatory disease
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.3324/haematol.2019.218545

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Role:
Author
ORCID:
0000-0002-4843-2975
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Role:
Author
ORCID:
0000-0002-1964-7133
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Role:
Author
ORCID:
0000-0002-7942-8127


Publisher:
Ferrata Storti Foundation
Journal:
Haematologica More from this journal
Volume:
106
Issue:
1
Pages:
208-219
Publication date:
2020-01-16
DOI:
EISSN:
1592-8721
ISSN:
0390-6078


Language:
English
Keywords:
Pubs id:
1158421
Local pid:
pubs:1158421
Source identifiers:
W3000362980
Deposit date:
2025-10-11
ARK identifier:
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