Alveolar niche disruption and aberrant epithelial reprogramming are early hallmarks of idiopathic pulmonary fibrosis

  1. Aurelien Justet
  2. Venerino Poletti
  3. Cristian Coarfa
  4. Nebal Abu Hussein
  5. Taylor Adams
  6. Alan Waich
  7. Agshin Balayev
  8. Xiting Yan
  9. Zhongyu Cai
  10. Farah Moussa
  11. Ruben De Man
  12. Johad Khoury
  13. Jonas C Schupp
  14. Juan D Zuluaga
  15. Amy Zhao
  16. Julian Villalba
  17. Farida Ahangari
  18. Scott A Ochsner
  19. Edward Manning
  20. Wendy J Introne
  21. Robert Homer
  22. Bernadette R Gochuico
  23. Laurens De Sadeleer
  24. Claudia Carducci
  25. Maria E Ruiz Echartea
  26. Chao He
  27. Bart M Vanaudenaerde
  28. Wim Wuyts
  29. Claudia Ravaglia
  30. Ivan Rosas
  31. Sara Tomassetti
  32. Naftali Kaminski
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Abstract

Idiopathic pulmonary fibrosis (IPF) is a progressive interstitial lung disease in which the earliest cellular events driving fibrosis remain poorly defined. Here, we analyzed lung samples from three independent and unique cohorts of patients with early disease and preserved lung function (Florence, NIH, Forli), applying an integrated multi-modal approach combining single-nucleus RNA sequencing, bulk transcriptomics, immunostaining, and spatial transcriptomics.

Single nuclear RNA sequencing of samples obtained by diagnostic bronchoscopic cryobiopsy (Florence, n= 22) revealed that early IPF is characterized by a marked shift in alveolar epithelial composition, with loss of AT1 and AT2 cells and the emergence of aberrant basaloid cells and alveolar epithelial intermediate cells. These populations exhibited transcriptional programs associated with epithelial plasticity and profibrotic signaling and closely resembled those observed in end-stage IPF. Higher proportions of aberrant basaloid and alveolar epithelial intermediate cells were associated with subsequent disease progression, whereas AT2 cell abundance correlated with preserved lung function. Fibrotic CTHRC1+ fibroblasts are largely restricted to advanced disease, while endothelial remodeling and inflammatory fibroblast states are already evident in early IPF. Spatial transcriptomic analyses confirmed early disruption of the alveolar niche, with replacement of normal epithelial–capillary interactions by aberrant epithelial and venous endothelial cells (Forli, n= 24); the findings were replicated through single cell RNA sequencing of samples obtained by video assisted thoracoscopy two decades earlier (NIH n=9).

Together, these findings identify that alveolar niche remodeling with loss of its normal components, and emergence of aberrant basaloid cells are features of early IPF, highlighting epithelial dysfunction as a key potential target for therapeutic interventions in early disease.

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  1. Version published to 10.64898/2026.05.27.727792 on bioRxiv