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西罗莫司洗脱支架断裂对 4 年临床结局的影响。

Impact of sirolimus-eluting stent fracture on 4-year clinical outcomes.

机构信息

Division of Cardiology, Toyota Memorial Hospital, 1-1 Heiwa-cho, Toyota, Japan.

出版信息

Circ Cardiovasc Interv. 2011 Aug;4(4):349-54. doi: 10.1161/CIRCINTERVENTIONS.110.958306. Epub 2011 Aug 2.

Abstract

BACKGROUND

Although stent fracture (SF) after sirolimus-eluting stent (SES) implantation has been recognized as one of the predisposing factors of in-stent restenosis, it remains uncertain whether SF can increase the risk of major adverse cardiac events (MACE), especially beyond 1 year after SES implantation. The aim of this study was to assess the impact of SF relative to non-SF on 4-year clinical outcomes after treatment with SES of comparable unselected lesions.

METHODS AND RESULTS

A total of 874 lesions in 793 patients undergoing SES implantation and subsequent angiography 6 to 9 months after index procedure were analyzed. At 6- to 9-month angiographic follow-up, SF was identified in 70 of 874 lesions (8.0%). In-stent late loss was significantly higher in SF lesions versus non-SF lesions (0.42±0.59 mm versus 0.13±0.49 mm, P<0.001), resulting in a significantly higher in-stent restenosis rate (21.4% versus 4.1%, P<0.001). At 4 years, SF versus non-SF was associated with a significantly higher MACE rate (23.2% versus 12.6%, P=0.014), mainly driven by significantly higher target-lesion revascularization (18.8% versus 10.2%, P=0.029) rate. Adverse effects of SF on clinical outcomes occurred mostly within the first year (17.4% versus 6.6%, P=0.001), with similar MACE rate between 1 and 4 years (5.8% versus 5.9%, P=0.611). No significant differences between SF versus non-SF patients were observed in the cumulative frequency of very late stent thrombosis (2.9% versus 1.4%, P=0.281), death (0% versus 2.1%, P=0.252), or myocardial infarction (5.8% versus 2.9%, P=0.165).

CONCLUSIONS

SF of SES was associated with higher MACE rate up to 1 year, mainly driven by higher target-lesion revascularization, whereas no significant association was evident between years 1 and 4.

摘要

背景

虽然支架断裂(SF)在雷帕霉素洗脱支架(SES)植入后已被认为是再狭窄的一个诱发因素,但SF 是否会增加主要不良心脏事件(MACE)的风险仍不确定,尤其是在 SES 植入后 1 年以上。本研究旨在评估与非 SF 相比,在接受 SES 治疗的可比未选择病变后 4 年的临床结果中 SF 的影响。

方法和结果

共分析了 793 例患者的 874 处病变,这些患者在指数手术后 6 至 9 个月接受了 SES 植入和随后的血管造影检查。在 6 至 9 个月的血管造影随访中,70 处病变(8.0%)发现有 SF。SF 病变的支架内晚期丢失明显高于非 SF 病变(0.42±0.59mm 比 0.13±0.49mm,P<0.001),导致支架内再狭窄率明显升高(21.4%比 4.1%,P<0.001)。4 年后,SF 与非 SF 相比,MACE 发生率明显更高(23.2%比 12.6%,P=0.014),主要是由于靶病变血运重建(18.8%比 10.2%,P=0.029)的发生率明显更高。SF 对临床结果的不良影响主要发生在第 1 年(17.4%比 6.6%,P=0.001),1 至 4 年的 MACE 发生率相似(5.8%比 5.9%,P=0.611)。SF 与非 SF 患者之间在累积极晚期支架血栓形成频率(2.9%比 1.4%,P=0.281)、死亡(0%比 2.1%,P=0.252)或心肌梗死(5.8%比 2.9%,P=0.165)方面无显著差异。

结论

SES 的 SF 与较高的 MACE 发生率相关,可达 1 年,主要是由于靶病变血运重建较高,而在第 1 年和第 4 年之间没有明显的相关性。

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