A Mouse Model of Vascular Injury that Induces Rapid Onset of Medial Cell Apoptosis Followed by Reproducible Neointimal Hyperplasia

新生内膜增生 再狭窄 管腔(解剖学) 内弹性层 血管成形术 医学 增生 股动脉 血管平滑肌 动脉 病变 转基因小鼠 解剖 病理 内科学 转基因 生物 支架 平滑肌 基因 生物化学
作者
M Sata,Y Maejima,F Adachi,K. Fukino,Akio Saiura,Seiryo Sugiura,Toshinori Aoyagi,Yasuo Imai,Hiroki Kurihara,Kiyoshi Kimura,Masao Omata,Masatoshi Makuuchi,Yasunobu Hirata,R Nagai
出处
期刊:Journal of Molecular and Cellular Cardiology [Elsevier BV]
卷期号:32 (11): 2097-2104 被引量:286
标识
DOI:10.1006/jmcc.2000.1238
摘要

Genetically modified mice serve as a powerful tool to determine the role of specific molecules in a wide variety of biological phenomena including vascular remodeling. Several models of arterial injury have been proposed to analyze transgenic/knock-out mice, but many questions have been raised about their reproducibility and physiological significance. Here, we report a new mouse model of vascular injury that resembles balloon-angioplasty. A straight spring wire was inserted into the femoral artery via arterioctomy in a small muscular branch. The wire was left in place for one minute to denude and dilate the artery. After the wire was removed, the muscular branch was tied off and the blood flow of the femoral artery was restored. The lumen was enlarged with rapid onset of medial cell apoptosis. While the circumference of the external elastic lamina remained enlarged, the lumen was gradually narrowed by neointimal hyperplasia composed of smooth muscle cells. At 4 weeks, a concentric and homogeneous neointimal lesion was formed reproducibly in the region where the wire had been inserted. Similar exuberant hyperplasia could be induced in all strains examined (C57BL/6J, C3H/HeJ, BALB/c, and 129/SVj). This model may be widely used to study the molecular mechanism of post-angioplasty restenosis at the genetic level.

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