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The characteristics of endothelial progenitor cells derived from mononuclear cells of rat bone marrow in different culture conditions

机译:不同培养条件下大鼠骨髓单核细胞来源的内皮祖细胞的特征

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Endothelial progenitor cells (EPCs) derived from bone marrow are known to be heterogeneous. In this study, we tried to find favorable conditions that induce the differentiation of mononuclear cells (MNCs) from bone marrow into EPCs. The differentiation capacity of MNCs from rat bone marrow was investigated in different conditions, such as different media, different induction times and different culture surfaces. The cell morphology and endothelial biomarkers associated with differentiated MNCs were studied. Our results indicated that MNCs cultured in EGM-2MV (Endothelial cell basal medium-2, plus SingleQuots of growth supplements) developed a bursiform shape, a late EPC-like morphology, while MNCs cultured in complete medium (CM, M199 with 10% FBS, 20 ng/mL VEGF and 10 ng/mL bFGF) showed a spindle shape, an early EPC-like morphology. Cells of both morphologies were able to incorporate DiI-ac-LDL and bind lectin in vitro. MNCs cultured in EGM-2MV exhibited a higher proliferation rate and higher eNOS expression than MNCs cultured in CM. MNCs cultured in EGM-2MV had the ability to form tubes on Matrigel. Flow cytometry results indicated that CD133 expression was highest at day 12 and that the greatest number of cells positive for both FLK-1 and CD133 appeared at day 20 from cells cultured in dishes without fibronectin coating. In addition, the expression levels of CD133, CD31 and FLK-1/CD133 were not significantly different between cells of different shapes. Our experiments suggest that MNCs from bone marrow can be differentiated into late EP-like cells in EGM-2MV, which have the ability to rapidly proliferate. These MNCs can also be differentiated into early EP-like cells in CM. Additionally, fibronectin may not be necessary for the differentiation of EPCs to mature ECs after three generations. Differentiated MNCs from bone marrow in EGM-2MV have the characteristics of EPCs, although the expression levels of EPC markers were lower than previously reported.
机译:已知源自骨髓的内皮祖细胞(EPC)是异质的。在这项研究中,我们试图找到有利的条件来诱导单核细胞(MNC)从骨髓分化为EPC。在不同条件下,例如不同的培养基,不同的诱导时间和不同的培养表面,研究了大鼠骨髓中MNC的分化能力。研究了与分化的MNC相关的细胞形态和内皮生物标志物。我们的结果表明,在EGM-2MV(内皮细胞基础培养基2,加上生长补充剂的单价)中培养的MNC形成了呈囊状,呈晚期EPC样的形态,而在完全培养基(CM,M199和10%FBS)中培养的MNC ,20 ng / mL VEGF和10 ng / mL bFGF)呈纺锤形,是早期的EPC样形态。两种形态的细胞都能够掺入DiI-ac-LDL并在体外结合凝集素。与在CM中培养的MNC相比,在EGM-2MV中培养的MNC表现出更高的增殖速率和更高的eNOS表达。在EGM-2MV中培养的MNC具有在Matrigel上形成管的能力。流式细胞术结果表明,在无纤连蛋白涂层的培养皿中培养的细胞,CD133的表达在第12天最高,而在FLK-1和CD133阳性的最大细胞数出现在第20天。另外,在不同形状的细胞之间,CD133,CD31和FLK-1 / CD133的表达水平没有显着差异。我们的实验表明,来自骨髓的MNC可以分化为EGM-2MV中的晚期EP样细胞,它们具有快速增殖的能力。这些MNC也可以在CM中分化成早期EP样细胞。另外,纤连蛋白对于三代后EPC分化为成熟EC可能不是必需的。尽管EPC标记的表达水平低于先前报道的水平,但EGM-2MV中与骨髓分化的MNC具有EPC的特征。

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