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支架小梁覆盖和内皮细胞覆盖:载有雷帕霉素的涂层和无涂层的金属裸支架与铂铬支架之间的比较。

Strut tissue coverage and endothelial cell coverage: a comparison between bare metal stent platforms and platinum chromium stents with and without everolimus-eluting coating.

机构信息

Boston Scientific Corporation, Natick, MA, USA.

出版信息

EuroIntervention. 2010 Nov;6(5):630-7. doi: 10.4244/EIJV6I5A105.

Abstract

AIMS

In a rabbit denudation model, assess impact of strut thickness on arterial healing by comparing endothelial cell coverage and strut tissue coverage after implantation of bare metal stents of varying thickness; evaluate the effect of an everolimus-eluting stent.

METHODS AND RESULTS

Strut tissue coverage and endothelialisation were assessed 14 and 21 days after implantation with scanning electron microscopy quantitation methods and immunostaining against the endothelial cell marker PECAM-1 (CD-31). At 14 days, strut tissue coverage was higher with the stainless steel Liberté stent (88%, 97 µm) versus Express (77%, 132 µm). The platinum chromium Element stent with the thinnest strut (81 µm) had the highest level (95%). By 21 days endothelialisation was complete for all. The everolimus-eluting Element stent had a 1-week delay in luminal endothelialisation but was >89% by 21 days; strut endothelial coverage was >79% in 80% (4/5) of animals, with total strut tissue coverage >95%.

CONCLUSIONS

This study demonstrated that strut thickness affects strut tissue coverage post stent implantation and the addition of an everolimus-eluting polymer introduces a short delay in endothelialisation. The results highlight the need to control for aspects of stent design such as strut thickness when comparing across drug-eluting stent platforms.

摘要

目的

在兔去内皮模型中,通过比较不同厚度裸金属支架植入后内皮细胞覆盖和支架组织覆盖情况,评估支柱厚度对动脉愈合的影响;评估依维莫司洗脱支架的效果。

方法和结果

植入后 14 天和 21 天采用扫描电子显微镜定量方法和针对内皮细胞标志物 PECAM-1(CD-31)的免疫染色评估支架组织覆盖和内皮化情况。在 14 天时,不锈钢 Liberté 支架(88%,97 µm)的支架组织覆盖高于 Express 支架(77%,132 µm)。最薄支柱(81 µm)的铂铬 Element 支架具有最高水平(95%)。21 天后,所有支架均完全内皮化。依维莫司洗脱 Element 支架的管腔内皮化延迟了 1 周,但在 21 天内超过 89%;80%(4/5)的动物中支架内皮覆盖率超过 79%,总支架组织覆盖率超过 95%。

结论

本研究表明,支柱厚度会影响支架植入后的支架组织覆盖情况,添加依维莫司洗脱聚合物会导致内皮化延迟。研究结果强调,在比较不同药物洗脱支架平台时,需要控制支架设计的方面,如支柱厚度。

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