生物
细胞生物学
粘液纤毛清除率
核糖核酸
细胞分化
细胞
免疫学
遗传学
肺
基因
语言学
哲学
作者
Sandra Ruiz García,Marie Deprez,Kévin Lebrigand,Amélie Cavard,Agnès Paquet,Marie‐Jeanne Arguel,Virginie Magnone,Marin Truchi,Ignacio Caballero,Sylvie Leroy,Charles‐Hugo Marquette,Brice Marcet,Pascal Barbry,Laure‐Emmanuelle Zaragosi
出处
期刊:Development
[The Company of Biologists]
日期:2019-09-26
卷期号:146 (20)
被引量:292
摘要
The upper airway epithelium, which is mainly composed of multiciliated, goblet, club and basal cells, ensures proper mucociliary function and can regenerate in response to assaults. In chronic airway diseases, defective repair leads to tissue remodeling. Delineating key drivers of differentiation dynamics can help understand how normal or pathological regeneration occurs. Using single-cell transcriptomics and lineage inference, we have unraveled trajectories from basal to luminal cells, providing novel markers for specific populations. We report that: (1) a precursor subgroup of multiciliated cells, which we have entitled deuterosomal cells, is defined by specific markers, such as DEUP1, FOXN4, YPEL1, HES6 and CDC20B; (2) goblet cells can be precursors of multiciliated cells, thus explaining the presence of hybrid cells that co-express markers of goblet and multiciliated cells; and (3) a repertoire of molecules involved in the regeneration process, such as keratins or components of the Notch, Wnt or BMP/TGFβ pathways, can be identified. Confirmation of our results on fresh human and pig airway samples, and on mouse tracheal cells, extend and confirm our conclusions regarding the molecular and cellular choreography at work during mucociliary epithelial differentiation.
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