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桡动脉支架内再狭窄的机制:一项猪实验研究。

The mechanism of in-stent restenosis in radius stent: an experimental porcine study.

作者信息

Iso Yoshitaka, Suzuki Hiroshi, Sato Takatoshi, Shoji Makoto, Shibata Masayuki, Shimizu Nobuyuki, Koba Shinji, Geshi Eiichi, Katagiri Takashi

机构信息

Third Department of Internal Medicine, Showa University School of Medicine, Tokyo, Japan.

出版信息

Circ J. 2005 Apr;69(4):481-7. doi: 10.1253/circj.69.481.

Abstract

BACKGROUND

We investigated the mechanism of in-stent restenosis in radius stents in comparison to balloon-expandable stent (NIR stent) in pigs, with a focus on extracellular matrix (ECM).

METHODS AND RESULTS

Radius (n = 4) or NIR (n = 4) stents were implanted in the left coronary arteries of miniature pigs. Quantitative coronary ultrasound (QCU) was performed before, immediately after, and at 1 and 4 weeks after the implantation. The stented-coronary arteries were harvested at 4 weeks after the implantation followed by immunohistochemical, histological, reverse transcription-polymerase chain reaction (RT-PCR) and real-time PCR studies. In QCU, mean luminal areas at 4 weeks did not differ between both groups, whereas the mean stent area and neointimal area were significantly greater in the radius (p < 0.01). The immunohistochemical study revealed a significantly decreased number of neointimal macrophages and neovascularizations (p < 0.05, p < 0.01, respectively), and a stronger expression of tenascin-C in the radius. The histological study showed a larger ECM area and less neointimal cell density in the radius than in the NIR. The RT-PCR and real-time PCR analysis revealed an enhanced expression of tanascin-C mRNA in the radius than in the NIR.

CONCLUSIONS

Increased production of ECM, especially tenascin-C, played a greater role in the neointimal formation in the radius stent than inflammation.

摘要

背景

我们研究了猪体内桡动脉支架与球囊扩张支架(NIR支架)相比发生支架内再狭窄的机制,重点关注细胞外基质(ECM)。

方法与结果

将桡动脉支架(n = 4)或NIR支架(n = 4)植入小型猪的左冠状动脉。在植入前、植入后即刻以及植入后1周和4周进行定量冠状动脉超声(QCU)检查。植入后4周采集带支架的冠状动脉,随后进行免疫组织化学、组织学、逆转录聚合酶链反应(RT-PCR)和实时PCR研究。在QCU检查中,两组在4周时的平均管腔面积无差异,而桡动脉支架组的平均支架面积和新生内膜面积显著更大(p < 0.01)。免疫组织化学研究显示,桡动脉支架组新生内膜巨噬细胞数量和新生血管形成显著减少(分别为p < 0.05,p < 0.01),且肌腱蛋白-C的表达更强。组织学研究表明,与NIR支架相比,桡动脉支架的ECM面积更大,新生内膜细胞密度更低。RT-PCR和实时PCR分析显示,桡动脉支架中肌腱蛋白-C mRNA的表达高于NIR支架。

结论

细胞外基质,尤其是肌腱蛋白-C的产生增加,在桡动脉支架新生内膜形成中比炎症起更大作用。

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