4.6 Article

Multiple Fibroblast Subtypes Contribute to Matrix Deposition in Pulmonary Fibrosis

Journal

Publisher

AMER THORACIC SOC
DOI: 10.1165/rcmb.2022-0292OC

Keywords

pulmonary fibrosis; fibroblast subtype; single-cell RNA-sequencing; cell surface marker; extracellular matrix

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This study identified and confirmed novel fibroblast subtypes in lung fibrosis through analyzing single-cell RNA sequencing data of mouse models and human lung fibrotic diseases. The researchers also identified specific cell surface proteins for each fibroblast subtype and found that lipofibroblasts and Ebf11 fibroblasts contribute to matrix deposition and possess enhanced invasive, proliferative, and contraction phenotypes. The study provides new insights for the development of therapeutics targeting lung fibroblast subtypes.
Progressive pulmonary fibrosis results from a dysfunctional tissue repair response and is characterized by fibroblast proliferation, activation, and invasion and extracellular matrix accumulation. Lung fibroblast heterogeneity is well recognized. With single-cell RNA sequencing, fibroblast subtypes have been reported by recent studies. However, the roles of fibroblast subtypes in effector functions in lung fibrosis are not well understood. In this study, we incorporated the recently published single-cell RNA-sequencing datasets on murine lung samples of fibrosis models and human lung samples of fibrotic diseases and analyzed fibroblast gene signatures. We identified and confirmed the novel fibroblast subtypes we reported recently across all samples of both mouse models and human lung fibrotic diseases, including idiopathic pulmonary fibrosis, systemic sclerosis-associated interstitial lung disease, and coronavirus disease (COVID-19). Furthermore, we identified specific cell surface proteins for each fibroblast subtype through differential gene expression analysis, which enabled us to isolate primary cells representing distinct fibroblast subtypes by flow cytometry sorting. We compared matrix production, including fibronectin, collagen, and hyaluronan, after profibrotic factor stimulation and assessed the invasive capacity of each fibroblast subtype. Our results suggest that in addition to myofibroblasts, lipofibroblasts and Ebf11 (Ebf transcription factor 11) fibroblasts are two important fibroblast subtypes that contribute to matrix deposition and also have enhanced invasive, proliferative, and contraction phenotypes. The histological locations of fibroblast subtypes are identified in healthy and fibrotic lungs by these cell surface proteins. This study provides new insights to inform approaches to targeting lung fibroblast subtypes to promote the development of therapeutics for lung fibrosis.

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