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Cangrelor resulted in inferior platelet aggregation inhibition compared with tirofiban in patients with STEMI who were undergoing PCI, the FABOLUS-FASTER study found.
The study, which was presented at the virtual PCR e-Course and simultaneously published in Circulation, also found that cangrelor (Kengreal, Chiesi) and tirofiban (Aggrastat, Medicure) generated greater platelet aggregation inhibition compared with chewed prasugrel (Effient, Daiichi Sankyo/Eli Lilly).
“The study shows for the first time that tirofiban is roughly threefold more potent in P2Y12 pathway inhibition than cangrelor, which was associated with surprisingly low levels of platelet inhibition,” Marco Valgimigli, MD, PhD, professor of cardiology and deputy chief at Cardiocentro Lugano in Switzerland, told Healio. “Chewed prasugrel has slightly better inhibition upfront, but there was mainly a marginal difference with integer prasugrel, which did not reach statistical significance. Hence, the bottom line is that even chewing oral P2Y12 inhibitors tablets does not really help to mitigate the platelet reactivity in the acute phase of a STEMI and that parenteral drugs are needed, but their comparative effectiveness differs substantially.”
Patients with STEMI
In this multicenter, open-label, randomized study, researchers analyzed data from 122 patients (mean age, 64 years; 76% men) with STEMI who underwent primary PCI between July 4, 2017, and Aug. 26, 2019, in three centers in Switzerland and Italy.
Patients were assigned standard regimen of tirofiban (n = 40; mean age, 63 years; 78% men), standard regimen of cangrelor (n = 40; mean age, 66 years; 73% men) or 60 mg prasugrel at PCI initiation. The prasugrel group were also assigned chewed (n = 21; mean age, 65 years; 90% men) or integral tablet administration (n = 21; mean age, 61 years; 67% men).
The primary endpoint was inhibition of platelet aggregation at 30 minutes at light transmittance aggregometry with 20 µmol/L of adenosine diphosphate.
Compared with tirofiban, cangrelor did not meet noninferiority. Patients assigned tirofiban had superior platelet aggregation inhibition compared with those assigned cangrelor (95 vs. 34.1; P < .001).
Tirofiban and cangrelor were superior to chewed prasugrel (10.5; P for both < .001). Compared with integral prasugrel, chewed prasugrel did not reach superior platelet aggregation inhibition (6.3; P = .47), although it resulted in higher active metabolite concentration (62.3 ng/mL vs. 17.1 ng/mL; P = .016).
“The data clearly speak for the fact that tirofiban is a much more potent antiplatelet agent in the acute phase of STEMI and should probably be preferred to cangrelor unless the bleeding risk remains a matter of concern, which, in the acute phase of STEMI, is clearly not frequently the case, whereas the ischemic risk is prevailing,” Valgimigli said in an interview.
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Additional research
Valgimigli said more research is needed in this area. “A study powered for overcome data would be highly desirable. A modern use of glycoprotein IIb/IIIa inhibitors consisting in bolus followed by no or very short infusion has a high potential for optimizing the ischemic risk without an excess of bleeding complications,” he said.
Reference:
Valgimigli M, et al. STEMI Interventions: First-in-Man and Novel Pharmacological Strategies. Presented at: PCR e-Course; June 25-27, 2020 (virtual meeting).