他汀类药物强度与外周动脉疾病股动脉支架一次通畅率之间的关系

IF 1.2 Q3 CARDIAC & CARDIOVASCULAR SYSTEMS CVIR Endovascular Pub Date : 2024-08-03 DOI:10.1186/s42155-024-00472-4
Elisabeth R. Seyferth, Helen Song, Ansar Z. Vance, Timothy W. I. Clark
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引用次数: 0

摘要

他汀类药物被广泛应用于冠状动脉和外周动脉疾病,但其对因外周动脉疾病而置入的支架的通畅性的影响尚未得到充分研究。本研究的目的是根据支架置入时他汀类药物的强度评估股动脉支架的主要通畅性,并将这种影响与可能影响支架通畅性的其他协变量进行比较。一项回顾性研究发现,216 名患者在 10 年间共置入了 278 个离散的股骨头支架;卢瑟福分类为 2(3.6%)、3(12.9%)、4(21.2%)、5(49.6%)和 6(12.6%)。支架位置为股总动脉(1.8%)、股总动脉/股浅动脉(0.7%)、股浅动脉(50.7%)、股浅动脉/腘动脉(32.7%)和腘动脉(14.0%);63.3%的支架为紫杉醇洗脱。每种支架结构的主要通畅性均通过双相超声、血管造影或计算机断层扫描血管造影来确定。50%以上的再狭窄或支架闭塞被视为丧失通畅性。Cox比例危险模型和Kaplan-Meier模型用于评估他汀类药物的使用和其他协变量对支架通畅性的影响。与未使用他汀类药物治疗的患者相比,置入支架时使用任何他汀类药物的患者丧失初级非辅助通畅的几率是后者的一半(危险比为 0.53;95% 置信区间为 0.19-0.87;P = .004)。与无他汀类药物治疗组相比,中度/高强度他汀类药物治疗可使支架中位通畅时间延长 17 个月。抗血小板治疗、抗凝治疗、药物洗脱支架(相对于裸金属或覆盖支架)和卢瑟福分级对支架通畅率没有预测作用(P = 0.52、0.85、0.58 和 0.82)。股腘支架置入时使用他汀类药物治疗是影响初治无辅助通畅率的最具预测性的检查变量。
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Association between statin intensity and femoropopliteal stent primary patency in peripheral arterial disease
Statins are widely used in coronary and peripheral arterial disease, but their impact on patency of stents placed for peripheral arterial disease is not well-studied. The purpose of this study was to evaluate femoropopliteal stent primary patency according to statin intensity at the time of stent placement and compare this effect to other covariates that may influence stent patency. A retrospective review identified 278 discrete femoropopliteal stent constructs placed in 216 patients over a 10-year period; Rutherford categories were 2 (3.6%), 3 (12.9%), 4 (21.2%), 5 (49.6%), and 6 (12.6%). Stent locations were common femoral (1.8%), common femoral/superficial femoral (0.7%), superficial femoral (50.7%), superficial femoral/popliteal (32.7%) and popliteal (14.0%) arteries; 63.3% of stents were paclitaxel-eluting. Primary patency of each stent construct was determined with duplex ultrasound, angiography, or computed tomographic angiography. Greater than 50% restenosis or stent occlusion was considered loss of patency. Cox proportional hazard and Kaplan–Meier modeling were used to assess the effect of statin use and additional covariates on stent patency. Patients on any statin at the time of stent placement were half as likely to undergo loss of primary unassisted patency as patients on no statin therapy (hazard ratio, 0.53; 95% confidence interval, 0.19–0.87; P = .004). Moderate/high intensity statin therapy conferred 17 additional months of median stent patency compared to the no statin group. Antiplatelet therapy, anticoagulant therapy, drug-eluting stents (versus bare metal or covered stents), and Rutherford class were not predictive of stent patency (P = 0.52, 0.85, 0.58, and 0.82, respectively). Use of statin therapy at the time of femoropopliteal stent placement was the most predictive examined variable influencing primary unassisted patency.
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来源期刊
CVIR Endovascular
CVIR Endovascular Medicine-Radiology, Nuclear Medicine and Imaging
CiteScore
2.30
自引率
0.00%
发文量
59
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