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对胎鼠肺中的细胞命运进行分析揭示了 TI 和 TII 细胞发育的不同途径。

Cell fate analysis in fetal mouse lung reveals distinct pathways for TI and TII cell development.

机构信息

Cardiovascular Research Institute, University of California, San Francisco, California.

Department of Pediatrics, University of California, San Francisco, California.

出版信息

Am J Physiol Lung Cell Mol Physiol. 2019 Nov 1;317(5):L653-L666. doi: 10.1152/ajplung.00503.2018. Epub 2019 Aug 21.

Abstract

Alveolar type I (TI) cells are large squamous cells that cover >95% of the internal surface area of the lung; type II (TII) cells are small cuboidal cells with distinctive intracellular surfactant storage organelles. Based on autoradiographic studies in the 1970s, the long-held paradigm of alveolar epithelial development has been a linear progression from undifferentiated progenitor cells through TII cells to TI cells. Subsequent data support the existence of more complex pathways. Recently, a bipotent TI/TII progenitor cell at embryonic day E18 has been inferred both from marker expression in developing airways and from statistical analyses of gene expression data obtained from single-lung embryonic cells. To study cell lineage directly by fate mapping, we developed new transgenic mouse models in which rtTA is driven either by the rat podoplanin or the mouse Sftpc gene to mark cells irreversibly in development. Using these models, we found two distinct lineage pathways. One pathway, evident as early as E12-15, is devoted almost exclusively to TI cell development; a second pathway gives rise predominantly to TII cells but also a subpopulation of TI cells. We have defined the molecular phenotypes of these distinct progenitor populations and have identified potential regulatory factors in TI and TII cell differentiation. By analyzing gene pathways in mature TI and TII cells, we identified potential novel functions of each cell type. These results provide novel insights into lung development and suggest a basis for testing strategies to promote alveolar differentiation and repair, including potential transplantation of lineage-specific progenitor cells.

摘要

肺泡 I 型(TI)细胞是覆盖肺内表面面积>95%的大型扁平细胞;II 型(TII)细胞是具有独特细胞内表面活性剂储存细胞器的小立方细胞。基于 20 世纪 70 年代的放射性自显影研究,肺泡上皮细胞发育的长期模式一直是从未分化的祖细胞通过 TII 细胞到 TI 细胞的线性进展。随后的数据支持更复杂途径的存在。最近,从发育中的气道中的标志物表达以及从单个肺胚胎细胞获得的基因表达数据的统计分析中,推断出胚胎第 18 天存在双能 TI/TII 祖细胞。为了通过命运图谱直接研究细胞谱系,我们开发了新的转基因小鼠模型,其中 rtTA 由大鼠 podoplanin 或小鼠 Sftpc 基因驱动,以在发育过程中不可逆地标记细胞。使用这些模型,我们发现了两种不同的谱系途径。一种途径早在 E12-15 就很明显,几乎专门用于 TI 细胞发育;第二种途径主要产生 TII 细胞,但也产生 TI 细胞的亚群。我们已经定义了这些不同祖细胞群体的分子表型,并鉴定了 TI 和 TII 细胞分化中的潜在调节因子。通过分析成熟 TI 和 TII 细胞中的基因途径,我们确定了每个细胞类型的潜在新功能。这些结果为肺发育提供了新的见解,并为测试促进肺泡分化和修复的策略提供了基础,包括潜在的谱系特异性祖细胞移植。

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