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Bone marrow-derived cells are not involved in reendothelialized endothelium as endothelial cells after simple endothelial denudation in mice

机译:小鼠简单内皮剥脱后,作为内皮细胞,骨髓来源的细胞不参与内皮细胞内皮化

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It has been shown that bone marrow (BM)-derived cells are involved in repaired endothelium induced by a model such as neointima-produced wire injury in mice. This has not been shown in a less invasive model that results in simple reendothelialization. A new wire-induced simple endothelial denudation model of the common carotid artery (CCA) of mice, which did not form neointima at 14 days after the operation, was established. At 7 days after operation, the CCAs were reendothelialized from the aortic arch and the carotid bifurcation but not completely, shown by whole-mount CD31 immunohistochemical staining. Scanning electron microscopy revealed that unendothelialized area was covered with platelets. To determine the involvement of BM-derived cells in the repaired endothelium, the wild-type (WT) C57BL/6 mice, in which BM cells derived from strain-matched green fluorescent protein (GFP)-transgenic mice were transplanted, were operated upon. As a result, there was no GFP-positive endothelial cell (EC) in reendothelialized endothelium, otherwise GFP-positive ‘dendritic’-like cells were recruited under the repaired endothelial layer. Administration of recombinant human erythropoietin [1,000 IU/(kg day) at 0–3 days after operation subcutaneously], which has been shown to increase endothelial progenitor cells in peripheral blood, also could not recruit BM-derived cells as ECs in BM-transplanted mice despite accelerating reendothelialization in WT mice [%reendothelialized area of the administrated group 78.0 ± 9.4% (mean ± SD) vs. the control group 63.0 ± 4.4%, P < 0.05]. These results suggest that BM-derived cells may not be involved in reendothelialization as ECs after simple endothelial denudation in mice.
机译:已经显示,骨髓(BM)衍生的细胞参与了由模型诱导的修复的内皮,所述模型例如由小鼠的新内膜产生的丝损伤。在侵入性较小的模型中并未显示出这一点,该模型可导致简单的内皮再形成。建立了一种新的线致小鼠颈总动脉(CCA)的简单血管内皮剥脱模型,该模型在术后14天没有形成新内膜。术后7天,CCA从主动脉弓和颈动脉分叉处重新内皮化,但不完全,这通过CD31免疫组化染色显示。扫描电子显微镜显示未内皮化的区域被血小板覆盖。为了确定BM来源的细胞在修复的内皮细胞中的参与程度,对野生型(WT)C57BL / 6小鼠进行了手术,在该小鼠中,移植了来自应变匹配的绿色荧光蛋白(GFP)-转基因小鼠的BM细胞。 。结果,在内皮内皮化的内皮细胞中没有GFP阳性内皮细胞(EC),否则在修复的内皮层下募集了GFP阳性“树突状”样细胞。重组人促红细胞生成素的给药[皮下手术后0至3天后为1,000 IU /(kg·day)],已显示可增加外周血中的内皮祖细胞,也不能募集BM来源的细胞作为BM移植的EC尽管在WT小鼠中内皮增生加速,小鼠[给药组的内皮增生面积百分比为78.​​0±9.4%(平均值±SD),而对照组为63.0±4.4%,P <0.05]。这些结果表明,在小鼠进行简单的内皮剥脱后,作为EC的BM来源的细胞可能不参与再内皮化。

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