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首页> 外文期刊>Tissue engineering, Part A >Human umbilical cord blood-derived cd34-positive endothelial progenitor cells stimulate osteoblastic differentiation of cultured human periosteal-derived osteoblasts
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Human umbilical cord blood-derived cd34-positive endothelial progenitor cells stimulate osteoblastic differentiation of cultured human periosteal-derived osteoblasts

机译:人脐血CD34阳性内皮祖细胞刺激培养的人骨膜来源成骨细胞的成骨分化

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摘要

The aim of this study was to examine the effects of human umbilical cord blood-derived CD34-positive endothelial progenitor cells (CD34+ EPCs) on osteoblastic differentiation of cultured human periosteal-derived osteoblasts (POs). CD34+ cells from human umbilical cord blood were sorted to purify more EPCs in characterization. These sorted cells showed CD31, VE-cadherin, and KDR expression as well as CD34 expression and formed typical tubes in Matrigel. These sorted cells were referred to as human cord blood-derived CD34+ EPCs. In in vivo bone formation using a miniature pig model, the newly formed bone was clearly examined in defects filled with polydioxanone/pluronic F127 (PDO/Pluronic F127) scaffolds containing either human umbilical cord blood-derived CD34+ EPCs and POs or human umbilical vein endothelial cells (HUVEC) and POs; however, the new bone had the greatest density in the defect treated with CD34+ EPCs and POs. Osteoblastic phenotypes of cultured human POs using ALP activity and von Kossa staining were also more clearly found in CD34+ EPC-conditioned medium than CD34-negative (CD34-) cell-conditioned medium, whereas HUVEC-conditioned medium had an intermediate effect. PCR array for common cytokines and growth factors showed that the secretion of interleukin (IL)-1β was significantly higher in CD34+ EPCs than in HUVEC, followed by level in CD34- cells. In addition, IL-1β also potently and dose dependently increased ALP activity and mineralization of POs in culture. These results suggest that human umbilical cord blood-derived CD34+ EPCs stimulates osteoblastic differentiation of cultured human POs. The functional role of human umbilical cord blood-derived CD34+ EPCs in increasing the osteogenic phenotypes of cultured human POs may depend on IL-1β secreted from human umbilical cord blood-derived CD34+ EPCs.
机译:这项研究的目的是检查人脐带血来源的CD34阳性内皮祖细胞(CD34 + EPC)对培养的人骨膜来源的成骨细胞(POs)成骨细胞分化的影响。从人脐带血中分离出CD34 +细胞,以纯化更多的EPC。这些分选的细胞显示CD31,VE-钙黏着蛋白和KDR表达以及CD34表达,并在Matrigel中形成典型的管。这些分选的细胞称为人脐带血CD34 + EPC。在使用微型猪模型的体内骨骼形成中,清楚地检查了新形成的骨骼中是否充满了聚二恶烷酮/普流尼克F127(PDO /普流尼克F127)支架的缺损,该支架中包含人脐带血CD34 + EPC和POs或人脐静脉内皮单元(HUVEC)和PO然而,新骨在用CD34 + EPC和POs治疗的缺损中密度最大。在CD34 + EPC条件培养基中,使用ALP活性和von Kossa染色培养的人POs的成骨细胞表型比CD34阴性(CD34-)细胞条件培养基更明显,而HUVEC条件培养基则具有中间作用。常见细胞因子和生长因子的PCR阵列显示,CD34 + EPC中白细胞介素(IL)-1β的分泌显着高于HUVEC,其次是CD34-细胞中的水平。另外,IL-1β还有效和剂量依赖性地增加了培养物中PO的ALP活性和矿化度。这些结果表明,人脐带血来源的CD34 + EPC刺激培养的人POs的成骨细胞分化。人脐带血来源的CD34 + EPC在增加培养的人PO的成骨表型中的功能性作用可能取决于人脐带血来源的CD34 + EPC分泌的IL-1β。

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