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首页> 外文期刊>Cell stem cell >The role of Scgb1a1+ Clara cells in the long-term maintenance and repair of lung airway, but not alveolar, epithelium.
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The role of Scgb1a1+ Clara cells in the long-term maintenance and repair of lung airway, but not alveolar, epithelium.

机译:Scgb1a1 + Clara细胞在肺气道(而非肺泡上皮)的长期维护和修复中的作用。

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To directly test the contribution of Scgb1a1(+) Clara cells to postnatal growth, homeostasis, and repair of lung epithelium, we generated a Scgb1a1-CreER knockin majority of Clara cells in the bronchioles both self-renews and generates ciliated cells. In the trachea, Clara cells give rise to ciliated cells but do not self-renew extensively. Nevertheless, they can contribute to tracheal repair. In the postnatal mouse lung, it has been proposed that bronchioalveolar stem cells (BASCs) which coexpress Scgb1a1 (Secretoglobin1a1) and SftpC (Surfactant Protein C), contribute descendants to both bronchioles and alveoli. The putative BASCs were lineage labeled in our studies. However, we find no evidence for the function of a special BASC population during postnatal growth, adult homeostasis, or repair. Rather, our results support a model in which the trachea, bronchioles, and alveoli are maintained by distinct populations of epithelial progenitor cells.
机译:为了直接测试Scgb1a1(+)Clara细胞对产后生长,体内稳态和肺上皮修复的贡献,我们在细支气管中生成了一个Scgb1a1-CreER敲入的大部分Clara细胞,它们既可以自我更新,又可以产生纤毛细胞。在气管中,克拉拉细胞会产生纤毛细胞,但不会大量自我更新。然而,它们可以有助于气管修复。在出生后的小鼠肺中,已经提出了共同表达Scgb1a1(Secretoglobin1a1)和SftpC(表面活性蛋白C)的支气管肺泡干细胞(BASC)有助于细支气管和肺泡。在我们的研究中,假定的BASC被谱系标记。但是,我们没有发现特殊的BASC人群在产后生长,成人体内稳态或修复过程中发挥功能的证据。相反,我们的结果支持一种模型,其中气管,细支气管和肺泡由上皮祖细胞的不同种群维持。

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