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首页> 外文期刊>Journal of biomaterials applications >Local delivery of nicotine does not mitigate fibrosis but may lead to angiogenesis.
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Local delivery of nicotine does not mitigate fibrosis but may lead to angiogenesis.

机译:尼古丁的局部递送不能减轻纤维化,但可能导致血管生成。

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摘要

As with most implanted biomaterials, the wound healing response following implantation of a silicone breast implant leads to the formation of a fibrotic capsule. This can result in capsular contracture, a painful complication that often necessitates the removal of implant. It is well established that nicotine and nicotinic agonists inhibit inflammatory signaling. Based on the link between the inflammatory response and capsule formation, we hypothesized that local delivery of nicotine from the implant may lead to the reduction in inflammation and capsule thickness, which may ultimately reduce the incidence of capsular contracture. Nicotine was loaded into PDMS membranes using a previously established method. The loaded materials were implanted into the submammary pockets between the third and fourth mammary glands of rats. To confirm that the nicotine was acting locally and not systemically, serum cotinine, the primary metabolite of nicotine, was measured by ELISA at 3 days. Thirty days post implantation, the animals were euthanized and the tissue samples were fixed for histological analysis. Blood vessel density was measured immunohistochemically, while the capsule thickness was evaluated microscopically. While the presence of the nicotine metabolite, cotinine, in the serum at the early time points demonstrated that the nicotine was released locally from the devices, there were no significant differences in the capsule thickness between the control and experimental implants. However, the results indicated that there were differences in angiogenesis with the local delivery of nicotine, which may have other implications for the development of biomaterials.
机译:与大多数植入的生物材料一样,硅酮乳房植入物植入后的伤口愈合反应导致纤维化囊的形成。这可能导致包膜挛缩,这是一种痛苦的并发症,通常需要去除植入物。众所周知,尼古丁和烟碱激动剂可以抑制炎症信号。基于炎症反应与包膜形成之间的联系,我们假设从植入物中局部输送尼古丁可导致炎症和包膜厚度减少,从而最终减少包膜挛缩的发生率。使用先前建立的方法将尼古丁加载到PDMS膜中。将负载的材料植入大鼠第三和第四乳腺之间的乳腺下袋中。为了确认尼古丁起局部作用而不是全身作用,在第3天通过ELISA测定了血清可替宁(尼古丁的主要代谢产物)。植入后三十天,对动物实施安乐死并固定组织样本以进行组织学分析。免疫组织化学测量血管密度,而显微镜下评估胶囊厚度。尽管早期时间点血清中存在尼古丁代谢物可替宁,表明尼古丁从装置中局部释放,但对照组和实验植入物之间的胶囊厚度没有显着差异。但是,结果表明,尼古丁的局部递送在血管生成方面存在差异,这可能对生物材料的开发有其他影响。

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