Effect of antiplatelet agents and tyrosine kinase inhibitors on oxLDL-mediated procoagulant platelet activity

Tony J. Zheng; Tia C.L. Kohs; Paul A. Mueller; Jiaqing Pang; Stéphanie E. Reitsma; Iván Parra-Izquierdo; Alexander R. Melrose; Liping Yang; Jaewoo Choi; Keith D. Zientek; Denis O. Sviridov; Mark K. Larson; Craig D. Williams; Nathalie Pamir; Joseph J. Shatzel; Ashok P. Reddy; Paul Kievit; Alan T. Remaley; Jan F. Stevens; Monica T. Hinds; Owen J.T. McCarty; Joseph E. Aslan

doi:10.1182/bloodadvances.2022007169

Effect of antiplatelet agents and tyrosine kinase inhibitors on oxLDL-mediated procoagulant platelet activity

Tony J. Zheng, Tia C.L. Kohs, Paul A. Mueller, Jiaqing Pang, Stéphanie E. Reitsma, Iván Parra-Izquierdo, Alexander R. Melrose, Liping Yang, Jaewoo Choi, Keith D. Zientek, Denis O. Sviridov, Mark K. Larson, Craig D. Williams, Nathalie Pamir, Joseph J. Shatzel, Ashok P. Reddy, Paul Kievit, Alan T. Remaley, Jan F. Stevens, Monica T. HindsOwen J.T. McCarty, Joseph E. Aslan

Research output: Contribution to journal › Article › peer-review

5 Scopus citations

Abstract

Low-density lipoprotein (LDL) contributes to atherogenesis and cardiovascular disease through interactions with peripheral blood cells, especially platelets. However, mechanisms by which LDL affects platelet activation and atherothrombosis, and how to best therapeutically target and safely prevent such responses remain unclear. Here, we investigate how oxidized low-density lipoprotein (oxLDL) enhances glycoprotein VI (GPVI)-mediated platelet hemostatic and procoagulant responses, and how traditional and emerging antiplatelet therapies affect oxLDL-enhanced platelet procoagulant activity ex vivo. Human platelets were treated with oxLDL and the GPVI-specific agonist, crosslinked collagen-related peptide, and assayed for hemostatic and procoagulant responses in the presence of inhibitors of purinergic receptors (P2YR), cyclooxygenase (COX), and tyrosine kinases. Ex vivo, oxLDL enhanced GPVI-mediated platelet dense granule secretion, a-granule secretion, integrin activation, thromboxane generation and aggregation, as well as procoagulant phosphatidylserine exposure and fibrin generation. Studies of washed human platelets, as well as platelets from mouse and nonhuman primate models of hyperlipidemia, further determined that P2YR antagonists (eg, ticagrelor) and Bruton tyrosine kinase inhibitors (eg, ibrutinib) reduced oxLDL-mediated platelet responses and procoagulant activity, whereas COX inhibitors (eg, aspirin) had no significant effect. Together, our results demonstrate that oxLDL enhances GPVI-mediated platelet procoagulant activity in a manner that may be more effectively reduced by P2YR antagonists and tyrosine kinase inhibitors compared with COX inhibitors.

Original language	English (US)
Pages (from-to)	1366-1378
Number of pages	13
Journal	Blood Advances
Volume	7
Issue number	8
DOIs	https://doi.org/10.1182/bloodadvances.2022007169
State	Published - Apr 25 2023

ASJC Scopus subject areas

Hematology

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10.1182/bloodadvances.2022007169

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Zheng, T. J., Kohs, T. C. L., Mueller, P. A., Pang, J., Reitsma, S. E., Parra-Izquierdo, I., Melrose, A. R., Yang, L., Choi, J., Zientek, K. D., Sviridov, D. O., Larson, M. K., Williams, C. D., Pamir, N., Shatzel, J. J., Reddy, A. P., Kievit, P., Remaley, A. T., Stevens, J. F., ... Aslan, J. E. (2023). Effect of antiplatelet agents and tyrosine kinase inhibitors on oxLDL-mediated procoagulant platelet activity. Blood Advances, 7(8), 1366-1378. https://doi.org/10.1182/bloodadvances.2022007169

Zheng, TJ, Kohs, TCL, Mueller, PA, Pang, J, Reitsma, SE, Parra-Izquierdo, I, Melrose, AR, Yang, L, Choi, J, Zientek, KD, Sviridov, DO, Larson, MK, Williams, CD, Pamir, N , Shatzel, JJ , Reddy, AP , Kievit, P, Remaley, AT, Stevens, JF, Hinds, MT , McCarty, OJT & Aslan, JE 2023, 'Effect of antiplatelet agents and tyrosine kinase inhibitors on oxLDL-mediated procoagulant platelet activity', Blood Advances, vol. 7, no. 8, pp. 1366-1378. https://doi.org/10.1182/bloodadvances.2022007169

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title = "Effect of antiplatelet agents and tyrosine kinase inhibitors on oxLDL-mediated procoagulant platelet activity",

abstract = "Low-density lipoprotein (LDL) contributes to atherogenesis and cardiovascular disease through interactions with peripheral blood cells, especially platelets. However, mechanisms by which LDL affects platelet activation and atherothrombosis, and how to best therapeutically target and safely prevent such responses remain unclear. Here, we investigate how oxidized low-density lipoprotein (oxLDL) enhances glycoprotein VI (GPVI)-mediated platelet hemostatic and procoagulant responses, and how traditional and emerging antiplatelet therapies affect oxLDL-enhanced platelet procoagulant activity ex vivo. Human platelets were treated with oxLDL and the GPVI-specific agonist, crosslinked collagen-related peptide, and assayed for hemostatic and procoagulant responses in the presence of inhibitors of purinergic receptors (P2YR), cyclooxygenase (COX), and tyrosine kinases. Ex vivo, oxLDL enhanced GPVI-mediated platelet dense granule secretion, a-granule secretion, integrin activation, thromboxane generation and aggregation, as well as procoagulant phosphatidylserine exposure and fibrin generation. Studies of washed human platelets, as well as platelets from mouse and nonhuman primate models of hyperlipidemia, further determined that P2YR antagonists (eg, ticagrelor) and Bruton tyrosine kinase inhibitors (eg, ibrutinib) reduced oxLDL-mediated platelet responses and procoagulant activity, whereas COX inhibitors (eg, aspirin) had no significant effect. Together, our results demonstrate that oxLDL enhances GPVI-mediated platelet procoagulant activity in a manner that may be more effectively reduced by P2YR antagonists and tyrosine kinase inhibitors compared with COX inhibitors.",

author = "Zheng, {Tony J.} and Kohs, {Tia C.L.} and Mueller, {Paul A.} and Jiaqing Pang and Reitsma, {St{\'e}phanie E.} and Iv{\'a}n Parra-Izquierdo and Melrose, {Alexander R.} and Liping Yang and Jaewoo Choi and Zientek, {Keith D.} and Sviridov, {Denis O.} and Larson, {Mark K.} and Williams, {Craig D.} and Nathalie Pamir and Shatzel, {Joseph J.} and Reddy, {Ashok P.} and Paul Kievit and Remaley, {Alan T.} and Stevens, {Jan F.} and Hinds, {Monica T.} and McCarty, {Owen J.T.} and Aslan, {Joseph E.}",

year = "2023",

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doi = "10.1182/bloodadvances.2022007169",

language = "English (US)",

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journal = "Blood Advances",

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T1 - Effect of antiplatelet agents and tyrosine kinase inhibitors on oxLDL-mediated procoagulant platelet activity

AU - Zheng, Tony J.

AU - Kohs, Tia C.L.

AU - Mueller, Paul A.

AU - Pang, Jiaqing

AU - Reitsma, Stéphanie E.

AU - Parra-Izquierdo, Iván

AU - Melrose, Alexander R.

AU - Yang, Liping

AU - Choi, Jaewoo

AU - Zientek, Keith D.

AU - Sviridov, Denis O.

AU - Larson, Mark K.

AU - Williams, Craig D.

AU - Pamir, Nathalie

AU - Shatzel, Joseph J.

AU - Reddy, Ashok P.

AU - Kievit, Paul

AU - Remaley, Alan T.

AU - Stevens, Jan F.

AU - Hinds, Monica T.

AU - McCarty, Owen J.T.

AU - Aslan, Joseph E.

PY - 2023/4/25

Y1 - 2023/4/25

N2 - Low-density lipoprotein (LDL) contributes to atherogenesis and cardiovascular disease through interactions with peripheral blood cells, especially platelets. However, mechanisms by which LDL affects platelet activation and atherothrombosis, and how to best therapeutically target and safely prevent such responses remain unclear. Here, we investigate how oxidized low-density lipoprotein (oxLDL) enhances glycoprotein VI (GPVI)-mediated platelet hemostatic and procoagulant responses, and how traditional and emerging antiplatelet therapies affect oxLDL-enhanced platelet procoagulant activity ex vivo. Human platelets were treated with oxLDL and the GPVI-specific agonist, crosslinked collagen-related peptide, and assayed for hemostatic and procoagulant responses in the presence of inhibitors of purinergic receptors (P2YR), cyclooxygenase (COX), and tyrosine kinases. Ex vivo, oxLDL enhanced GPVI-mediated platelet dense granule secretion, a-granule secretion, integrin activation, thromboxane generation and aggregation, as well as procoagulant phosphatidylserine exposure and fibrin generation. Studies of washed human platelets, as well as platelets from mouse and nonhuman primate models of hyperlipidemia, further determined that P2YR antagonists (eg, ticagrelor) and Bruton tyrosine kinase inhibitors (eg, ibrutinib) reduced oxLDL-mediated platelet responses and procoagulant activity, whereas COX inhibitors (eg, aspirin) had no significant effect. Together, our results demonstrate that oxLDL enhances GPVI-mediated platelet procoagulant activity in a manner that may be more effectively reduced by P2YR antagonists and tyrosine kinase inhibitors compared with COX inhibitors.

AB - Low-density lipoprotein (LDL) contributes to atherogenesis and cardiovascular disease through interactions with peripheral blood cells, especially platelets. However, mechanisms by which LDL affects platelet activation and atherothrombosis, and how to best therapeutically target and safely prevent such responses remain unclear. Here, we investigate how oxidized low-density lipoprotein (oxLDL) enhances glycoprotein VI (GPVI)-mediated platelet hemostatic and procoagulant responses, and how traditional and emerging antiplatelet therapies affect oxLDL-enhanced platelet procoagulant activity ex vivo. Human platelets were treated with oxLDL and the GPVI-specific agonist, crosslinked collagen-related peptide, and assayed for hemostatic and procoagulant responses in the presence of inhibitors of purinergic receptors (P2YR), cyclooxygenase (COX), and tyrosine kinases. Ex vivo, oxLDL enhanced GPVI-mediated platelet dense granule secretion, a-granule secretion, integrin activation, thromboxane generation and aggregation, as well as procoagulant phosphatidylserine exposure and fibrin generation. Studies of washed human platelets, as well as platelets from mouse and nonhuman primate models of hyperlipidemia, further determined that P2YR antagonists (eg, ticagrelor) and Bruton tyrosine kinase inhibitors (eg, ibrutinib) reduced oxLDL-mediated platelet responses and procoagulant activity, whereas COX inhibitors (eg, aspirin) had no significant effect. Together, our results demonstrate that oxLDL enhances GPVI-mediated platelet procoagulant activity in a manner that may be more effectively reduced by P2YR antagonists and tyrosine kinase inhibitors compared with COX inhibitors.

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SN - 2473-9529

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EP - 1378

JO - Blood Advances

JF - Blood Advances

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ER -

Effect of antiplatelet agents and tyrosine kinase inhibitors on oxLDL-mediated procoagulant platelet activity

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