Sfrp1 inhibits lung fibroblast invasion during transition to injury-induced myofibroblasts

Christoph H. Mayr(Zero to Three), Arunima Sengupta(Zero to Three), Sara Asgharpour(German Center for Lung Research), Meshal Ansari(Helmholtz Zentrum München), Jeanine C. Pestoni(German Center for Lung Research), Paulina Ogar(German Center for Lung Research), Ilias Angelidis(German Center for Lung Research), Andreas Liontos(Stockholm University), José Alberto Rodríguez‐Castillo(Max Planck Institute for Heart and Lung Research), Niklas J. Lang(German Center for Lung Research), Maximilian Strunz(German Center for Lung Research), Diana Porras-Gonzalez(German Center for Lung Research), Michael Gerckens(German Center for Lung Research), Laurens De Sadeleer(German Center for Lung Research), Bettina Oehrle(German Center for Lung Research), Valeria Viteri-Alvarez(German Center for Lung Research), Isis E. Fernandez(German Center for Lung Research), Michelle D. Tallquist(University of Hawaiʻi at Mānoa), Martin Irmler(Helmholtz Zentrum München), Johannes Beckers(Helmholtz Zentrum München), Oliver Eickelberg(University of Pittsburgh), Gabriel Stoleriu(German Center for Lung Research), Jürgen Behr(German Center for Lung Research), Nikolaus Kneidinger(German Center for Lung Research), Wim Wuyts(KU Leuven), Roxana Wasnick(German Center for Lung Research), Ali Önder Yildirim(German Center for Lung Research), Katrin Ahlbrecht(Max Planck Institute for Heart and Lung Research), Rory E. Morty(Heidelberg University), Christos Samakovlis(Stockholm University), Fabian J. Theis(Helmholtz Zentrum München), Gerald Burgstaller(Association for Symbolic Logic), Herbert B. Schiller(Association for Symbolic Logic)
European Respiratory Journal
January 11, 2024
10.1183/13993003.01326-2023
Cited by 99Open Access
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Abstract

Background Fibroblast-to-myofibroblast conversion is a major driver of tissue remodelling in organ fibrosis. Distinct lineages of fibroblasts support homeostatic tissue niche functions, yet their specific activation states and phenotypic trajectories during injury and repair have remained unclear. Methods We combined spatial transcriptomics, multiplexed immunostainings, longitudinal single-cell RNA-sequencing and genetic lineage tracing to study fibroblast fates during mouse lung regeneration. Our findings were validated in idiopathic pulmonary fibrosis patient tissues in situ as well as in cell differentiation and invasion assays using patient lung fibroblasts. Cell differentiation and invasion assays established a function of SFRP1 in regulating human lung fibroblast invasion in response to transforming growth factor (TGF)β1. Measurements and main results We discovered a transitional fibroblast state characterised by high Sfrp1 expression, derived from both Tcf21 -Cre lineage positive and negative cells. Sfrp1 + cells appeared early after injury in peribronchiolar, adventitial and alveolar locations and preceded the emergence of myofibroblasts. We identified lineage-specific paracrine signals and inferred converging transcriptional trajectories towards Sfrp1 + transitional fibroblasts and Cthrc1 + myofibroblasts. TGFβ1 downregulated SFRP1 in noninvasive transitional cells and induced their switch to an invasive CTHRC1 + myofibroblast identity. Finally, using loss-of-function studies we showed that SFRP1 modulates TGFβ1-induced fibroblast invasion and RHOA pathway activity. Conclusions Our study reveals the convergence of spatially and transcriptionally distinct fibroblast lineages into transcriptionally uniform myofibroblasts and identifies SFRP1 as a modulator of TGFβ1-driven fibroblast phenotypes in fibrogenesis. These findings are relevant in the context of therapeutic interventions that aim at limiting or reversing fibroblast foci formation.

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