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Neovascularization and vascular markers in a foreign body reaction to subcutaneously implanted degradable biomaterial in mice.

机译:小鼠皮下植入可降解生物材料的异物反应中的新血管形成和血管标志物。

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摘要

To study the spatiotemporal processes of angiogenesis during a foreign body reaction (FBR), biodegradable bovine collagen type-1 (COL-I) discs were implanted in mice for a period up to 28 days. The cellular infiltration (consisting mainly of macrophages, giant cells and fibroblasts), and the extent of neovascularization into the discs were determined. Also the expression levels and/or distribution of the endothelial cell markers von Willebrand factor (vWF), platelet endothelial cell adhesion molecule-1 (PECAM-1)/CD31, MECA-32 antigens and endomucin, and of the basal lamina marker collagen type IV (Coll IV) were analysed. In time, a strong neovascularization of the discs was observed, with frequently occurring vascular sprouting, and intussusceptive growth of vessels. In this model, vWF, MECA-32 and endomucin antibodies often failed to stain neovessels in the COL-I discs. In contrast, staining for collagen IV basal lamina component in combination with CD31 covered the complete range of neo-vessels. We conclude that the model described in this study is a useful model to study FBR induced angiogenesis because of the active neovascularization taking place during prolonged periods of time.
机译:为了研究异物反应(FBR)过程中血管生成的时空过程,将可生物降解的1型牛胶原蛋白(COL-1)光盘植入小鼠体内长达28天。确定了细胞浸润(主要由巨噬细胞,巨细胞和成纤维细胞组成)和新血管形成盘的程度。内皮细胞标记物von Willebrand因子(vWF),血小板内皮细胞粘附分子-1(PECAM-1)/ CD31,MECA-32抗原和内粘蛋白的表达水平和/或分布,以及基底层标记物胶原蛋白的表达水平和/或分布IV(Coll IV)进行了分析。随着时间的推移,观察到椎间盘强烈的新生血管形成,并经常发生血管发芽和血管套叠生长。在该模型中,vWF,MECA-32和内粘蛋白抗体通常无法染色COL-1盘中的新血管。相比之下,胶原IV基底层成分与CD31结合的染色覆盖了新血管的完整范围。我们得出的结论是,该研究中描述的模型是研究FBR诱导的血管生成的有用模型,因为在长时间内会发生活跃的新血管形成。

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