@article{06722678f7e44f47ad7a489cb8f4de64,
title = "Ibrutinib Inhibits BMX-Dependent Endothelial VCAM-1 Expression In Vitro and Pro-Atherosclerotic Endothelial Activation and Platelet Adhesion In Vivo",
abstract = "Introduction: Inflammatory activation of the vascular endothelium leads to overexpression of adhesion molecules such as vascular cell adhesion molecule-1 (VCAM-1), contributing to the pro-thrombotic state underpinning atherogenesis. While the role of TEC family kinases (TFKs) in mediating inflammatory cell and platelet activation is well defined, the role of TFKs in vascular endothelial activation remains unclear. We investigated the role of TFKs in endothelial cell activation in vitro and in a nonhuman primate model of diet-induced atherosclerosis in vivo. Methods and Results: In vitro, we found that ibrutinib blocked activation of the TFK member, BMX, by vascular endothelial growth factors (VEGF)-A in human aortic endothelial cells (HAECs). Blockade of BMX activation with ibrutinib or pharmacologically distinct BMX inhibitors eliminated the ability of VEGF-A to stimulate VCAM-1 expression in HAECs. We validated that treatment with ibrutinib inhibited TFK-mediated platelet activation and aggregation in both human and primate samples as measured using flow cytometry and light transmission aggregometry. We utilized contrast-enhanced ultrasound molecular imaging to measure platelet GPIbα and endothelial VCAM-1 expression in atherosclerosis-prone carotid arteries of obese nonhuman primates. We observed that the TFK inhibitor, ibrutinib, inhibited platelet deposition and endothelial cell activation in vivo. Conclusion: Herein we found that VEGF-A signals through BMX to induce VCAM-1 expression in endothelial cells, and that VCAM-1 expression is sensitive to ibrutinib in vitro and in atherosclerosis-prone carotid arteries in vivo. These findings suggest that TFKs may contribute to the pathogenesis of atherosclerosis and could represent a novel therapeutic target.",
keywords = "Atherosclerosis, BMX, BTK, Endothelial cell, Ibrutinib, Platelet, TEC, Tyrosine kinase",
author = "Kohs, {Tia C.L.} and Olson, {Sven R.} and Jiaqing Pang and Jordan, {Kelley R.} and Zheng, {Tony J.} and Aris Xie and James Hodovan and Matthew Muller and Carrie McArthur and Jennifer Johnson and Sousa, {B{\'a}rbara B.} and Michael Wallisch and Paul Kievit and Aslan, {Joseph E.} and Seixas, {Jo{\~a}o D.} and Bernardes, {Gon{\c c}alo J.L.} and Hinds, {Monica T.} and Lindner, {Jonathan R.} and McCarty, {Owen J.T.} and Cristina Puy and Shatzel, {Joseph J.}",
note = "Funding Information: This work has been supported by grants from the National Institute of Health (R01HL101972, R01HL078610, R01HL130046, R01HL151367, P51OD011092). The Endocrine Technologies Core and Clinical Pathology Laboratory is supported (in part) by a National Institute of Health grant (P51OD011092) for operation of the ONPRC. Funding Information: We thank Dr. Gray D. Shaw from Quell Pharma, Inc. for providing the GPIbα ligand and Dr. Richard W. Farndale from Cambridge University for providing the GPVI agonist, CRP-XL. T.C.L. Kohs, S.R. Olson, O.J.T. McCarty, and C. Puy, and J.J. Shatzel were responsible for project concept and design. A. Xie, J. Hodovan, M. Muller, C. McArthur, P. Kievit, M.T. Hinds, and J.R. Lindner executed primate studies. T.C.L. Kohs, J. Pang, K.R. Jordan, J. Johnson, M. Wallisch, J.E. Aslan, and C. Puy contributed in vitro data acquisition and analysis. B.B. Sousa, J.D. Seixas, and G.J.L. Bernardes provided the TFK inhibitor, JS25, and assisted with the structural biochemistry. T.C.L. Kohs and J.J. Shatzel drafted the manuscript. T.J. Zheng. S.R. Olson, and O.J.T. McCarty critically reviewed the manuscript. This work has been supported by grants from the National Institute of Health (R01HL101972, R01HL078610, R01HL130046, R01HL151367, P51OD011092). The Endocrine Technologies Core and Clinical Pathology Laboratory is supported (in part) by a National Institute of Health grant (P51OD011092) for operation of the ONPRC. M. Wallisch is an employee of Aronora, Inc., a company that may have a commercial interest in the results of this study. J.J. Shatzel reports receiving consulting fees from Aronora, Inc. The Oregon Health & Science University Conflict of Interest in Research Committee has reviewed and managed this potential conflict of interest. J.D. Seixas and G.J.L. Bernardes are the inventors of JS25 (Patent Application Number: 1908171.0). T.C.L. Kohs, S.R. Olson, J. Pang, K.R. Jordan, T.J. Zheng, A. Xie, J. Hodovan, M. Muller, C. McArthur, J. Johnson, B.B. Sousa, P. Kievit, J.E. Aslan, M.T. Hinds, J.R. Lindner, O.J.T. McCarty, and C. Puy declare no potential conflict of interest. All procedures followed were in accordance with the ethical standards of the responsible committee on human experimentation (institutional and national) and with the Helsinki Declaration of 1975, as revised in 2000 (5). All institutional and national guidelines for the care and use of laboratory animals were followed and approved by the Oregon Health & Science University Institutional Animal Care and Use Committee. Informed consent was obtained from all patients for being included in the study. Publisher Copyright: {\textcopyright} 2022, The Author(s) under exclusive licence to Biomedical Engineering Society.",
year = "2022",
month = jun,
doi = "10.1007/s12195-022-00723-1",
language = "English (US)",
volume = "15",
pages = "231--243",
journal = "Cellular and Molecular Bioengineering",
issn = "1865-5025",
publisher = "Springer New York",
number = "3",
}