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首页> 外文期刊>American Journal of Physiology >Targeted cell replacement with bone marrow cells for airway epithelial regeneration.
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Targeted cell replacement with bone marrow cells for airway epithelial regeneration.

机译:用骨髓细胞靶向性置换细胞,用于气道上皮再生。

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It has been suggested that some adult bone marrow cells (BMC) can localize to the lung and develop tissue-specific characteristics including those of pulmonary epithelial cells. Here, we show that the combination of mild airway injury (naphthalene-induced) as a conditioning regimen to direct the site of BMC localization and transtracheal delivery of short-term cultured BMC enhances airway localization and adoption of an epithelial-like phenotype. Confocal analysis of airway and alveolar-localized BMC (fluorescently labeled) with epithelial markers shows expression of the pulmonary epithelial proteins, Clara cell secretory protein, and surfactant protein C. To confirm epithelial gene expression by BMC, we generated transgenic mice expressing green fluorescent protein (GFP) driven by the epithelial-specific cytokeratin-18 promoter and injected BMC from these mice transtracheally into wild-type recipients after naphthalene-induced airway injury. BMC retention in the lung was observed for at least 120 daysfollowing cell delivery with increasing GFP transgene expression over time. Some BMC cultured in vitro over time also expressed GFP transgene, suggesting epithelial transdifferentiation of the BMC. The results indicate that targeted delivery of BMC can promote airway regeneration.
机译:已经提出,一些成年骨髓细胞(BMC)可以定位于肺并发展组织特异性特征,包括肺上皮细胞的特征。在这里,我们表明轻度气道损伤(萘引起)作为指导BMC定位和短期培养的BMC经气管递送的条件的调理方案的组合增强了气道定位和上皮样表型的采用。用上皮标记对气道和肺泡定位的BMC(荧光标记)进行共聚焦分析,显示肺上皮蛋白,Clara细胞分泌蛋白和表面活性剂蛋白C的表达。为了通过BMC确认上皮基因表达,我们生成了表达绿色荧光蛋白的转基因小鼠(GFP)由上皮特异性cytokeratin-18启动子驱动,并在萘诱导的气道损伤后经气管插管将这些小鼠的BMC气管内注入野生型受体。在细胞递送后至少120天观察到BMC保留在肺中,随着时间的推移GFP转基因表达增加。随着时间的推移体外培养的一些BMC也表达GFP转基因,表明BMC的上皮转分化。结果表明BMC的靶向递送可以促进气道再生。

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