van Overhagen Hans, Nakamura Masato, Geraghty Patrick J, Rao Sid, Arroyo Max, Soga Yoshimitsu, Iida Osamu, Armstrong Ehrin, Nakama Tatsuya, Fujihara Masahiko, Ansari Mohammad M, Mathews Santhosh J, Gouëffic Yann, Jaff Michael R, Weinberg Ido, Pinto Duane S, Ohura Norihiko, Couch Kara, Mustapha Jihad A
Haga Teaching Hospital, Den Haag, South Holland, The Netherlands.
Toho University Ohashi Medical Center, Meguro, Tokyo, Japan.
Vasc Med. 2023 Dec;28(6):571-580. doi: 10.1177/1358863X231199489. Epub 2023 Oct 16.
Effective and durable options for infrapopliteal artery revascularization for patients with chronic limb-threatening ischemia (CLTI) are limited.
The SAVAL trial is a prospective, multicenter, randomized trial of patients with CLTI and infrapopliteal artery lesions with total lesion length ⩽ 140 mm, stenosis ⩾ 70%, and Rutherford category 4-5 assigned 2:1 to treatment with the SAVAL self-expandable paclitaxel drug-eluting stent (DES) or percutaneous transluminal angioplasty (PTA) with an uncoated balloon. The primary effectiveness endpoint was primary vessel patency (i.e., core lab-adjudicated duplex ultrasound-based flow at 12 months in the absence of clinically driven target lesion revascularization or surgical bypass of the target lesion). The primary safety endpoint was the 12-month major adverse event (MAE)-free rate; MAEs were defined as a composite of above-ankle index limb amputation, major reintervention, and 30-day mortality. The endpoints were prespecified for superiority (effectiveness) and noninferiority (safety) at a one-sided significance level of 2.5%.
A total of 201 patients were enrolled and randomly assigned to treatment ( = 130 DES, = 71 PTA). Target lesion length was 68.1 ± 35.2 mm for the DES group and 68.7 ± 49.2 mm for the PTA group, and 31.0% and 27.6% of patients, respectively, had occlusions. The 12-month primary patency rates were 68.0% for the DES group and 76.0% for the PTA group (P = 0.8552). The MAE-free rates were 91.6% and 95.3%, respectively (P = 0.0433).
The SAVAL trial did not show benefit related to effectiveness and safety with the nitinol DES compared with PTA in infrapopliteal artery lesions up to 140 mm in length. Continued innovation to provide optimal treatments for CLTI is needed. .
对于慢性肢体威胁性缺血(CLTI)患者,腘下动脉血运重建的有效且持久的选择有限。
SAVAL试验是一项前瞻性、多中心、随机试验,纳入CLTI且腘下动脉病变、总病变长度≤140mm、狭窄≥70%以及卢瑟福分级为4 - 5级的患者,按2:1随机分配至接受SAVAL自膨胀紫杉醇药物洗脱支架(DES)治疗或使用无涂层球囊的经皮腔内血管成形术(PTA)治疗。主要有效性终点是主要血管通畅率(即核心实验室判定的基于双功超声的12个月时血流情况,且无临床驱动的靶病变血运重建或靶病变的外科搭桥)。主要安全性终点是12个月无主要不良事件(MAE)发生率;MAE定义为踝上指数肢体截肢、主要再次干预和30天死亡率的复合指标。这些终点在单侧显著性水平为2.5%时预先设定为优效性(有效性)和非劣效性(安全性)。
共纳入201例患者并随机分配至治疗组(DES组130例,PTA组71例)。DES组靶病变长度为68.1±35.2mm,PTA组为68.7±49.2mm,分别有31.0%和27.6% 的患者存在闭塞病变。DES组12个月主要通畅率为68.0%,PTA组为76.0%(P = 0.8552)。无MAE发生率分别为91.6%和95.3%(P = 0.0433)。
SAVAL试验未显示在长度达140mm的腘下动脉病变中,与PTA相比,镍钛合金DES在有效性和安全性方面有优势。需要持续创新以提供针对CLTI的最佳治疗方法。
