Application of Auxiliary VerifyNow Point-of-Care Assays to Assess the Pharmacodynamics of RUC-4, a Novel αIIbβ3 Receptor Antagonist
Introduction Prehospital therapy of ST-elevation myocardial infarction (STEMI) with αIIbβ3 antagonists improves clinical outcomes, but they are difficult to use in prehospital settings. RUC-4 is a novel αIIbβ3 antagonist being developed for prehospital therapy of STEMI that rapidly achieves high-gra...
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doaj-44739d156a174cadbbd7ae35ef38e4b82021-09-28T23:03:52ZengGeorg Thieme Verlag KGTH Open2512-94652021-07-010503e449e46010.1055/s-0041-1732343Application of Auxiliary VerifyNow Point-of-Care Assays to Assess the Pharmacodynamics of RUC-4, a Novel αIIbβ3 Receptor AntagonistOhad S. Bentur0Jihong Li1Caroline S. Jiang2Linda H. Martin3Dean J. Kereiakes4Barry S. Coller5Allen and Frances Adler Laboratory of Blood and Vascular Biology, Rockefeller University, New York, New York, United StatesAllen and Frances Adler Laboratory of Blood and Vascular Biology, Rockefeller University, New York, New York, United StatesThe Rockefeller University Hospital, New York, New York, United StatesThe Carl and Edyth Lindner Center for Research and Education at the Christ Hospital, Cincinnati, Ohio, United StatesThe Carl and Edyth Lindner Center for Research and Education at the Christ Hospital, Cincinnati, Ohio, United StatesAllen and Frances Adler Laboratory of Blood and Vascular Biology, Rockefeller University, New York, New York, United StatesIntroduction Prehospital therapy of ST-elevation myocardial infarction (STEMI) with αIIbβ3 antagonists improves clinical outcomes, but they are difficult to use in prehospital settings. RUC-4 is a novel αIIbβ3 antagonist being developed for prehospital therapy of STEMI that rapidly achieves high-grade platelet inhibition after subcutaneous administration. Standard light transmission aggregometry (LTA) is difficult to perform during STEMI, so we applied VerifyNow (VN) assays to assess the pharmacodynamics of RUC-4 relative to aspirin and ticagrelor. Methods Blood from healthy volunteers was anticoagulated with phenylalanyl-prolyl-arginyl chloromethyl ketone (PPACK) or sodium citrate, treated in vitro with RUC-4, aspirin, and/or ticagrelor, and tested with the VN ADP + PGE1, iso-TRAP, and base channel (high concentration iso-TRAP + PAR-4 agonist) assays. The results were correlated with both ADP (20 µM)-induced LTA and flow cytometry measurement of receptor occupancy and data from individuals treated in vivo with RUC-4. Results RUC-4 inhibited all three VN assays, aspirin did not affect the assays, and ticagrelor markedly inhibited the ADP + PGE1 assay, slightly inhibited the iso-TRAP assay, and did not inhibit the base channel assay. RUC-4's antiplatelet effects were potentiated in citrate compared with PPACK. Cut-off values were determined to correlate the results of the VN iso-TRAP and base channel assays with 80% inhibition of LTA. Conclusion The VN assays can differentiate the early potent anti-αIIbβ3 effects of RUC-4 from delayed effects of P2Y12 antagonists in the presence of aspirin. These pharmacodynamic assays can help guide the clinical development of RUC-4 and potentially be used to monitor RUC-4's effects in clinical practice.http://www.thieme-connect.de/DOI/DOI?10.1055/s-0041-1732343stemiplatelet aggregation inhibitorspoint-of-care testingplatelet glycoprotein gpiib-iiia complexacute myocardial infarction |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Ohad S. Bentur Jihong Li Caroline S. Jiang Linda H. Martin Dean J. Kereiakes Barry S. Coller |
spellingShingle |
Ohad S. Bentur Jihong Li Caroline S. Jiang Linda H. Martin Dean J. Kereiakes Barry S. Coller Application of Auxiliary VerifyNow Point-of-Care Assays to Assess the Pharmacodynamics of RUC-4, a Novel αIIbβ3 Receptor Antagonist TH Open stemi platelet aggregation inhibitors point-of-care testing platelet glycoprotein gpiib-iiia complex acute myocardial infarction |
author_facet |
Ohad S. Bentur Jihong Li Caroline S. Jiang Linda H. Martin Dean J. Kereiakes Barry S. Coller |
author_sort |
Ohad S. Bentur |
title |
Application of Auxiliary VerifyNow Point-of-Care Assays to Assess the Pharmacodynamics of RUC-4, a Novel αIIbβ3 Receptor Antagonist |
title_short |
Application of Auxiliary VerifyNow Point-of-Care Assays to Assess the Pharmacodynamics of RUC-4, a Novel αIIbβ3 Receptor Antagonist |
title_full |
Application of Auxiliary VerifyNow Point-of-Care Assays to Assess the Pharmacodynamics of RUC-4, a Novel αIIbβ3 Receptor Antagonist |
title_fullStr |
Application of Auxiliary VerifyNow Point-of-Care Assays to Assess the Pharmacodynamics of RUC-4, a Novel αIIbβ3 Receptor Antagonist |
title_full_unstemmed |
Application of Auxiliary VerifyNow Point-of-Care Assays to Assess the Pharmacodynamics of RUC-4, a Novel αIIbβ3 Receptor Antagonist |
title_sort |
application of auxiliary verifynow point-of-care assays to assess the pharmacodynamics of ruc-4, a novel αiibβ3 receptor antagonist |
publisher |
Georg Thieme Verlag KG |
series |
TH Open |
issn |
2512-9465 |
publishDate |
2021-07-01 |
description |
Introduction Prehospital therapy of ST-elevation myocardial infarction (STEMI) with αIIbβ3 antagonists improves clinical outcomes, but they are difficult to use in prehospital settings. RUC-4 is a novel αIIbβ3 antagonist being developed for prehospital therapy of STEMI that rapidly achieves high-grade platelet inhibition after subcutaneous administration. Standard light transmission aggregometry (LTA) is difficult to perform during STEMI, so we applied VerifyNow (VN) assays to assess the pharmacodynamics of RUC-4 relative to aspirin and ticagrelor.
Methods Blood from healthy volunteers was anticoagulated with phenylalanyl-prolyl-arginyl chloromethyl ketone (PPACK) or sodium citrate, treated in vitro with RUC-4, aspirin, and/or ticagrelor, and tested with the VN ADP + PGE1, iso-TRAP, and base channel (high concentration iso-TRAP + PAR-4 agonist) assays. The results were correlated with both ADP (20 µM)-induced LTA and flow cytometry measurement of receptor occupancy and data from individuals treated in vivo with RUC-4.
Results RUC-4 inhibited all three VN assays, aspirin did not affect the assays, and ticagrelor markedly inhibited the ADP + PGE1 assay, slightly inhibited the iso-TRAP assay, and did not inhibit the base channel assay. RUC-4's antiplatelet effects were potentiated in citrate compared with PPACK. Cut-off values were determined to correlate the results of the VN iso-TRAP and base channel assays with 80% inhibition of LTA.
Conclusion The VN assays can differentiate the early potent anti-αIIbβ3 effects of RUC-4 from delayed effects of P2Y12 antagonists in the presence of aspirin. These pharmacodynamic assays can help guide the clinical development of RUC-4 and potentially be used to monitor RUC-4's effects in clinical practice. |
topic |
stemi platelet aggregation inhibitors point-of-care testing platelet glycoprotein gpiib-iiia complex acute myocardial infarction |
url |
http://www.thieme-connect.de/DOI/DOI?10.1055/s-0041-1732343 |
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