A fibroblast-dependent TGF-β1/sFRP2 noncanonical Wnt signaling axis promotes epithelial metaplasia in idiopathic pulmonary fibrosis
Max L. Cohen, … , Harold A. Chapman, Claude Jourdan Le Saux
Max L. Cohen, … , Harold A. Chapman, Claude Jourdan Le Saux
Published July 9, 2024
Citation Information: J Clin Invest. 2024;134(18):e174598. https://doi.org/10.1172/JCI174598.
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A fibroblast-dependent TGF-β1/sFRP2 noncanonical Wnt signaling axis promotes epithelial metaplasia in idiopathic pulmonary fibrosis

Abstract

Reciprocal interactions between alveolar fibroblasts and epithelial cells are crucial for lung homeostasis, injury repair, and fibrogenesis, but underlying mechanisms remain unclear. To investigate, we administered the fibroblast-selective TGF-β1 signaling inhibitor epigallocatechin gallate (EGCG) to interstitial lung disease (ILD) patients undergoing diagnostic lung biopsy and conducted single-cell RNA-Seq on spare tissue. Biopsies from untreated patients showed higher fibroblast TGF-β1 signaling compared with nondisease donor or end-stage ILD tissues. In vivo, EGCG downregulated TGF-β1 signaling and several proinflammatory and stress pathways in biopsy samples. Notably, EGCG reduced fibroblast secreted frizzled-related protein 2 (sFRP2), an unrecognized TGF-β1 fibroblast target gene induced near type II alveolar epithelial cells (AEC2s) in situ. Using AEC2-fibroblast coculture organoids and precision-cut lung slices (PCLSs) from nondiseased donors, we found TGF-β1 signaling promotes a spread AEC2 KRT17+ basaloid state, whereupon sFRP2 then activates a mature cytokeratin 5+ (Krt5+) basal cell program. Wnt-receptor Frizzled 5 (Fzd5) expression and downstream calcineurin signaling were required for sFRP2-induced nuclear NFATc3 accumulation and KRT5 expression. These findings highlight stage-specific TGF-β1 signaling in ILD and the therapeutic potential of EGCG in reducing idiopathic pulmonary fibrosis–related (IPF-related) transcriptional changes and identify TGF-β1/noncanonical Wnt pathway crosstalk via sFRP2 as a mechanism for dysfunctional epithelial signaling in IPF/ILD.

Authors

Max L. Cohen, Alexis N. Brumwell, Tsung Che Ho, Kiana Garakani, Genevieve Montas, Darren Leong, Vivianne W. Ding, Jeffrey A. Golden, Binh N. Trinh, David M. Jablons, Michael A. Matthay, Kirk D. Jones, Paul J. Wolters, Ying Wei, Harold A. Chapman, Claude Jourdan Le Saux

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Figure 2

EGCG inhibits TGF-β1 pathway activity in fibroblasts from ILD biopsies and identifies sFRP2 as a downstream target gene.

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EGCG inhibits TGF-β1 pathway activity in fibroblasts from ILD biopsies a...
(A) Dimensional reduction plot of subsetted and reclustered alveolar (red) and pathologic (blue) (CTHRC1+, inflammatory, and HAS1+/BMP antagonist+) fibroblast subtypes from untreated biopsy (5,225 cells, n = 3) and EGCG biopsy (6,773 cells, n = 4) samples. (B) Volcano plot of differentially expressed genes in alveolar and pathologic fibroblast subtypes from EGCG biopsy versus untreated biopsy samples, with selected TGF-β pathway genes labeled, including sFRP2. (C) Heatmap of z scores from IPA upstream pathway analysis of differentially expressed genes in alveolar and pathologic fibroblast subtypes from EGCG biopsy versus untreated biopsy samples. (D) Violin plots of selected TGF-β pathway genes split by individual biopsy sample.