Persistence of a regeneration-associated, transitional alveolar epithelial cell state in pulmonary fibrosis

被引:0
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作者
Yoshihiko Kobayashi
Aleksandra Tata
Arvind Konkimalla
Hiroaki Katsura
Rebecca F. Lee
Jianhong Ou
Nicholas E. Banovich
Jonathan A. Kropski
Purushothama Rao Tata
机构
[1] Duke University School of Medicine,Department of Cell Biology
[2] Duke University School of Medicine,Medical Scientist Training Program
[3] Duke University,Regeneration Next
[4] Translational Genomics Research Institute,Division of Allergy, Pulmonary and Critical Care Medicine, Department of Medicine
[5] Vanderbilt University Medical Center,Department of Cell and Developmental Biology
[6] Department of Veterans Affairs Medical Center,Duke Cancer Institute
[7] Vanderbilt University,undefined
[8] Duke University School of Medicine,undefined
来源
Nature Cell Biology | 2020年 / 22卷
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摘要
Stem cells undergo dynamic changes in response to injury to regenerate lost cells. However, the identity of transitional states and the mechanisms that drive their trajectories remain understudied. Using lung organoids, multiple in vivo repair models, single-cell transcriptomics and lineage tracing, we find that alveolar type-2 epithelial cells undergoing differentiation into type-1 cells acquire pre-alveolar type-1 transitional cell state (PATS) en route to terminal maturation. Transitional cells undergo extensive stretching during differentiation, making them vulnerable to DNA damage. Cells in the PATS show an enrichment of TP53, TGFβ, DNA-damage-response signalling and cellular senescence. Gain and loss of function as well as genomic binding assays revealed a direct transcriptional control of PATS by TP53 signalling. Notably, accumulation of PATS-like cells in human fibrotic lungs was observed, suggesting persistence of the transitional state in fibrosis. Our study thus implicates a transient state associated with senescence in normal epithelial tissue repair and its abnormal persistence in disease conditions.
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页码:934 / 946
页数:12
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