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锌依赖性抑制可生物降解锌植入物的血管平滑肌内膜增生。

Zn-dependent suppression of vascular smooth muscle intimal hyperplasia from biodegradable zinc implants.

机构信息

Department of Biomedical Engineering, Michigan Technological University, USA.

Department of Biomedical Engineering, Michigan Technological University, USA.

出版信息

Mater Sci Eng C Mater Biol Appl. 2020 Jun;111:110826. doi: 10.1016/j.msec.2020.110826. Epub 2020 Mar 7.

Abstract

Biodegradable arterial implants based on zinc have been found to suppress neointimal hyperplasia, suggesting that biodegradable materials containing zinc may be used to construct vascular implants with a reduced rate of restenosis. However, the molecular mechanism has remained unclear. In this report, we show that zinc-containing materials can be used to prevent neointimal formation when implanted into the rat aorta. Indeed, neointimal cells were significantly more TUNEL positive and alpha-actin negative at the interface of biodegradable zinc vs. biostable platinum implants, in association with greater caspase-3 activity. Although zinc stimulated extensive neointimal smooth muscle cell (SMC) death, macrophage and proinflammatory markers CD68 and iNOS were not increased in neointimal tissue relative to biostable platinum control implants. Using arterial explants, ionic zinc was confirmed to promote SMC apoptosis by activating the caspase apoptotic signaling pathway. These observations suggest that zinc-containing materials can be used to construct vascular implants such as stents with reduced neointimal hyperplasia.

摘要

基于锌的可生物降解动脉植入物已被发现可抑制新生内膜增生,这表明含锌的可生物降解材料可用于构建再狭窄发生率降低的血管植入物。然而,其分子机制仍不清楚。在本报告中,我们表明,当将含锌材料植入大鼠主动脉时,可用于预防新生内膜形成。实际上,与生物稳定的铂植入物相比,可生物降解的锌植入物界面处的新生内膜细胞 TUNEL 阳性和α-肌动蛋白阴性更明显,同时 caspase-3 活性更高。尽管锌刺激了广泛的新生内膜平滑肌细胞(SMC)死亡,但与生物稳定的铂对照植入物相比,新生内膜组织中巨噬细胞和促炎标志物 CD68 和 iNOS 并未增加。使用动脉外植体,证实离子锌通过激活 caspase 凋亡信号通路促进 SMC 凋亡。这些观察结果表明,含锌材料可用于构建具有降低的新生内膜增生的血管植入物,例如支架。

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本文引用的文献

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