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西罗莫司洗脱支架和紫杉醇洗脱支架晚期管腔丢失模式的血管造影分析

Angiographic analysis of pattern of late luminal loss in sirolimus- and paclitaxel-eluting stents.

作者信息

Agostoni Pierfrancesco, Cosgrave John, Biondi-Zoccai Giuseppe G L, Sangiorgi Giuseppe M, Ge Lei, Melzi Gloria, Corbett Simon, Airoldi Flavio, Montorfano Matteo, Chieffo Alaide, Michev Iassen, Carlino Mauro, Colombo Antonio

机构信息

San Raffaele Hospital, Milan, Italy.

出版信息

Am J Cardiol. 2007 Mar 1;99(5):593-8. doi: 10.1016/j.amjcard.2006.09.104. Epub 2007 Jan 4.

Abstract

Late loss is becoming an important end point to compare drug-eluting stents; however, little is known about its pattern of distribution. We analyzed the pattern of late loss distribution in sirolimus-eluting stents (SESs) and paclitaxel-eluting stents (PESs) in a consecutive cohort of patients. From a cohort of 529 patients treated with drug-eluting stents in 1 year, we selected all patients who underwent angiographic follow-up. Three hundred fifty-nine patients with 592 de novo lesions received SESs (286 lesions) or PESs (306 lesions). Late loss and binary angiographic restenosis were analyzed. Binary restenosis occurred in 56 lesions (19.6%) treated with SESs compared with 53 (17.3%) treated with PESs (p = 0.48). The 2 late loss distributions were skewed to the right and were not normally distributed (p <0.001 for SES, p = 0.003 for PES). Late loss was significantly lower in the SES group (p = 0.03), with a median value of 0.29 mm (interquartile range -0.09 to 0.66) versus 0.41 mm (-0.02 to 0.85) in the PES group. When analyzing only restenotic lesions, late loss had a normal distribution in the SES and PES groups (p = 0.96 and 0.44, respectively) and was similar in the 2 groups (1.75 +/- 0.51 vs 1.82 +/- 0.62, p = 0.48). When evaluating nonrestenotic lesions, late loss was also normally distributed in the 2 groups (p = 0.75 for SES, p = 0.73 for PES) but was significantly lower (p = 0.002) after SES implantation (0.14 +/- 0.39) than after PES implantation (0.27 +/- 0.44). In conclusion, SESs and PESs have a bimodal pattern of late loss distribution. The observed difference in late loss between SES and PES seems to be partly explained by the decrease in late loss after SES implantation in nonrestenotic lesions (where SES approaches "zero late loss"). Thus, late loss may not be a reliable marker of the true efficacy of these devices due to its complex and nongaussian distribution.

摘要

晚期管腔丢失正逐渐成为比较药物洗脱支架的一个重要终点;然而,对于其分布模式却知之甚少。我们分析了连续一组患者中雷帕霉素洗脱支架(SES)和紫杉醇洗脱支架(PES)的晚期管腔丢失分布模式。在1年中接受药物洗脱支架治疗的529例患者队列中,我们选取了所有接受血管造影随访的患者。359例患者的592处初发病变接受了SES(286处病变)或PES(306处病变)治疗。分析了晚期管腔丢失和二元血管造影再狭窄情况。SES治疗的56处病变(19.6%)发生了二元再狭窄,而PES治疗的为53处(17.3%)(p = 0.48)。两种晚期管腔丢失分布均向右偏斜,且非正态分布(SES的p <0.001,PES的p = 0.003)。SES组的晚期管腔丢失显著更低(p = 0.03),中位数为0.29 mm(四分位间距为 -0.09至0.66),而PES组为0.41 mm(-0.02至0.85)。仅分析再狭窄病变时,SES组和PES组的晚期管腔丢失呈正态分布(分别为p = 0.96和0.44),且两组相似(1.75±0.51对1.82±0.62,p = 0.48)。评估非再狭窄病变时,两组的晚期管腔丢失也呈正态分布(SES的p = 0.75,PES的p = 0.73),但SES植入后(0.14±0.39)显著低于PES植入后(0.27±0.44)(p = 0.002)。总之,SES和PES具有双峰型的晚期管腔丢失分布模式。SES和PES之间观察到的晚期管腔丢失差异似乎部分可由非再狭窄病变中SES植入后晚期管腔丢失的减少来解释(SES接近“零晚期管腔丢失”)。因此,由于晚期管腔丢失的复杂和非高斯分布,它可能不是这些器械真正疗效的可靠标志物。

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