Department of Advanced Biomedical Sciences, Federico II University of Naples, Naples, Italy.
Department of Translational Medical Sciences, University of Campania "Luigi Vanvitelli", Naples, Italy; Division of Cardiology, A.O.R.N. "Sant'Anna e San Sebastiano", Caserta, Italy.
Am Heart J. 2023 Nov;265:153-160. doi: 10.1016/j.ahj.2023.08.001. Epub 2023 Aug 10.
Over the past few decades, percutaneous coronary intervention (PCI) has undergone significant advancements as a result of the combination of device-based and drug-based therapies. These iterations have led to the development of polymer-free drug-eluting stents. However, there is a scarcity of data regarding their clinical performance. Furthermore, while various risk scores have been proposed to determine the optimal duration of dual antiplatelet therapy (DAPT), none of them have undergone prospective validation within the context of randomized trials.
The PARTHENOPE trial is a phase IV, prospective, randomized, multicenter, investigator-initiated, assessor-blind study being conducted at 14 centers in Italy (NCT04135989). It includes 2,107 all-comers patients with minimal exclusion criteria, randomly assigned in a 2-by-2 design to receive either the Cre8 amphilimus-eluting stent or the SYNERGY everolimus-eluting stent, along with either a personalized or standard duration of DAPT. Personalized DAPT duration is determined by the DAPT score, which accounts for both bleeding and ischemic risks. Patients with a DAPT score <2 (indicating higher bleeding than ischemic risk) receive DAPT for 3 or 6 months for chronic or acute coronary syndrome, respectively, while patients with a DAPT score ≥2 (indicating higher ischemic than bleeding risk) receive DAPT for 24 months. Patients in the standard DAPT group receive DAPT for 12 months. The trial aims to establish the noninferiority between stents with respect to a device-oriented composite end point of cardiovascular death, target-vessel myocardial infarction, or clinically-driven target-lesion revascularization at 12 months after PCI. Additionally, the trial aims to demonstrate the superiority of personalized DAPT compared to a standard approach with respect to a net clinical composite of all-cause death, any myocardial infarction, stroke, urgent target-vessel revascularization, or type 2 to 5 bleeding according to the Bleeding Academic Research Consortium criteria at 24-months after PCI.
The PARTHENOPE trial is the largest randomized trial investigating the efficacy and safety of a polymer-free DES with a reservoir technology for drug-release and the first trial evaluating a personalized duration of DAPT based on the DAPT score. The study results will provide novel insights into the optimizing the use of drug-eluting stents and DAPT in patients undergoing PCI.
在过去几十年中,由于器械和药物治疗的结合,经皮冠状动脉介入治疗(PCI)取得了重大进展。这些迭代导致了无聚合物药物洗脱支架的发展。然而,关于它们的临床性能的数据却很少。此外,尽管已经提出了各种风险评分来确定双联抗血小板治疗(DAPT)的最佳持续时间,但没有一个在随机试验的背景下经过前瞻性验证。
PARTHENOPE 试验是一项四期、前瞻性、随机、多中心、研究者发起、评估者盲法研究,在意大利的 14 个中心进行(NCT04135989)。它包括 2107 名各种类型的患者,最小的排除标准,以 2×2 的设计随机分配接受 Cre8 依维莫司洗脱支架或 SYNERGY 依维莫司洗脱支架,以及个性化或标准的 DAPT 持续时间。个性化 DAPT 持续时间由 DAPT 评分决定,该评分同时考虑出血和缺血风险。DAPT 评分<2 的患者(表示出血风险高于缺血风险)分别接受 3 或 6 个月的 DAPT 治疗,用于慢性或急性冠状动脉综合征,而 DAPT 评分≥2 的患者(表示缺血风险高于出血风险)接受 24 个月的 DAPT 治疗。标准 DAPT 组的患者接受 12 个月的 DAPT。该试验旨在确定支架在 PCI 后 12 个月时,以心血管死亡、靶血管心肌梗死或临床驱动的靶病变血运重建为导向的器械复合终点方面的非劣效性。此外,该试验旨在证明与标准方法相比,基于 DAPT 评分的个体化 DAPT 在 PCI 后 24 个月时,根据 Bleeding Academic Research Consortium 标准的全因死亡、任何心肌梗死、卒中和紧急靶血管血运重建或 2 至 5 型出血的净临床复合终点方面具有优越性。
PARTHENOPE 试验是最大的随机试验,研究了具有储库技术的无聚合物 DES 的疗效和安全性,用于药物释放,也是第一个根据 DAPT 评分评估个体化 DAPT 持续时间的试验。研究结果将为优化 PCI 患者使用药物洗脱支架和 DAPT 提供新的见解。
