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Prospective Isolation of Bronchiolar Stem Cells Based Upon Immunophenotypic and Autofluorescence Characteristics §

机译:基于免疫表型和自身荧光特征的细支气管干细胞的前瞻性分离 §

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Bronchiolar stem cells have been functionally defined in vivo on the basis of their resistance to chemical (naphthalene) injury, their infrequent proliferation relative to other progenitor cell types, and their coexpression of the airway and alveolar secretory cell markers Clara cell secretory protein and pro-surfactant protein C, respectively. Cell surface markers that have previously been used for their prospective isolation included Sca-1 and CD34. Using transgenic animal models associated with stem cell expansion, ablation, and lineage tracing, we demonstrate that CD34pos cells do not belong to the airway epithelial lineage and that cell surface Sca-1 immunoreactivity does not distinguish between bronchiolar stem and facultative transit-amplifying (Clara) cell populations. Furthermore, we show that high autofluorescence (AFhigh) is a distinguishing characteristic of Clara cells allowing for the fractionation of AFlow bronchiolar stem cells. On the basis of these data we show that the defining phenotype of the bronchiolar stem cell is CD45neg CD31neg CD34neg Sca-llow AFlow. This refinement in the definition of bronchiolar stem cells provides a critical tool by which to assess functional and molecular distinctions between bronchiolar stem cells and the more abundant pool of facultative transit-amplifying (Clara) cells. STEM CELLS 2009;27:612-622
机译:细支气管干细胞在体内的功能定义是基于其对化学(萘)损伤的抗性,相对于其他祖细胞类型的不常见增殖以及它们与气道和肺泡分泌细胞标志物共表达的Clara细胞分泌蛋白和pro-表面活性剂蛋白C分别。先前已用于前瞻性分离的细胞表面标记包括Sca-1和CD34。使用与干细胞扩增,消融和谱系追踪相关的转基因动物模型,我们证明CD34pos细胞不属于气道上皮谱系,并且细胞表面Sca-1免疫反应性不能区分细支气管干和兼性转运扩增(Clara )细胞群体。此外,我们表明,高自发荧光(AFhigh)是Clara细胞的显着特征,允许分流AFlow细支气管干细胞。根据这些数据,我们显示细支气管干细胞的定义表型是CD45neg CD31neg CD34neg Sca-low AFlow。细支气管干细胞定义的这种改进提供了一种关键工具,通过该工具可以评估细支气管干细胞与兼性转运扩增(Clara)细胞池之间的功能和分子差异。干细胞2009; 27:612-622

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    《STEM CELLS 》 |2009年第3期| 612-622| 共11页
  • 作者单位

    Division of Pulmonary, Allergy and Critical Care, Duke University Medical Center, Durham, North Carolina, USA|Department of Environmental and Occupational Health, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, USA;

    McGowan Institute for Regenerative Medicine, University of Pittsburgh, Pittsburgh, Pennsylvania, USA;

    Human Vaccine Institute, Duke University Medical Center, Durham, North Carolina, USA;

    Division of Pulmonary, Allergy and Critical Care, Duke University Medical Center, Durham, North Carolina, USA|Department of Environmental and Occupational Health, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, USA;

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