PAR-1 antagonist vorapaxar favorably improves global thrombotic status in patients with coronary disease
| Autor: | Robert G. Wilcox, G. Rosser, Pierluigi Tricoci, David A. Morrow, Maria Niespialowska-Steuden, C. Christopoulos, Diana A. Gorog, Robert Kozarski |
|---|---|
| Rok vydání: | 2014 |
| Předmět: |
Male
medicine.medical_specialty Pyridines medicine.medical_treatment Coronary Disease Placebo Lactones Double-Blind Method Interquartile range Internal medicine medicine Humans Receptor PAR-1 Longitudinal Studies Platelet activation Thrombus Aged Vorapaxar business.industry Thrombosis Hematology Thrombolysis Middle Aged medicine.disease Surgery Cardiology Female Cardiology and Cardiovascular Medicine Off Treatment business medicine.drug |
| Zdroj: | Journal of Thrombosis and Thrombolysis. 38:423-429 |
| ISSN: | 1573-742X 0929-5305 |
| Popis: | To assess the effect of vorapaxar on global thrombotic and thrombolytic status. The propensity for thrombus formation is determined by the balance between prothrombotic factors and endogenous thrombolysis. Impaired thrombolytic status increases cardiovascular risk. Vorapaxar is a novel, oral, protease-activated receptor-1 antagonist that inhibits thrombin-induced platelet activation. In the TRACER and TRA 2°P-TIMI 50 studies, patients with acute coronary syndromes and established atherosclerosis were randomized to vorapaxar 2.5 mg daily or placebo, in addition to standard care. In 57 patients enrolled in a single center, blood was tested with the point-of-care global thrombosis test, on and off treatment. This automated test employs non-anticoagulated blood to assess thrombotic and thrombolytic status, measuring the time required to form a shear-induced thrombus under physiological conditions (occlusion time, OT), and subsequently, the time to achieve endogenous lysis of the thrombus (lysis time, LT). Patients on vorapaxar exhibited longer OT on vs. off treatment [median 561 s (interquartile range 422-654) vs. 372 s(338-454), P = 0.003] and shorter LT on treatment than off [1,158 s(746-1,492) vs. 1,733 s(1,388-2,230), P = 0.016]. Patients on placebo showed no difference in OT [419 s(343-514) vs. 411 s(346-535), P = 0.658] or LT [1,236 s(985-1,594) vs. 1,400 s(1,092-1,686), P = 0.524] on and off treatment. During treatment, OT was longer in patients taking vorapaxar [561 s(422-654) vs. 419 s(343-514), P = 0.009], but LT was similar in vorapaxar and placebo arms [1,158 s(746-1,492) vs. 1,236 s(985-1,594), P = 0.277]. Vorapaxar prolongs OT and shortens LT, with favorable effects on thrombotic and thrombolytic status. In addition to its antiplatelet effect, vorapaxar may enhance endogenous thrombolysis, which is frequently impaired in coronary disease. |
| Databáze: | OpenAIRE |
| Externí odkaz: |
|
Full text from SpringerLink