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Epithelial cell derived lumican modulates extracellular matrix dynamics in early-life airways disease - 05/01/26

Doi : 10.1016/j.jaci.2025.08.030 
Franz Puttur, PhD a, , William J. Traves, MSc a, Minerva G. Martin, MSc a, Samuele Di Carmine, MSc b, Frédéric Fercoq, PhD c, David C.A. Gaboriau, PhD d, Lewis J. Entwistle, PhD a, Laura Yates, PhD a, Régis Joulia, PhD a, Sara Patti, MSc a, Helen Stölting, PhD a, Ciara Campbell, MSc a, Mindy L. Gore, PhD a, Simone A. Walker, MSc a, Lola E. Loewenthal, MD a, f, Philip L. Molyneaux, MD a, f, Leo M. Carlin, PhD c, e, Sejal Saglani, MD a, f, Clare M. Lloyd, PhD a,
a National Heart and Lung Institute, Imperial College London, London, United Kingdom 
b School of Life Sciences, University of Dundee, Dundee, United Kingdom 
c Cancer Research UK Scotland Institute, Glasgow, United Kingdom 
d Facility for Imaging by Light Microscopy, National Heart and Lung Institute, Imperial College London, London, United Kingdom 
e School of Cancer Sciences, University of Glasgow, Glasgow, United Kingdom 
f Royal Brompton and Harefield Hospitals, Guy’s and St Thomas’ NHS Foundation Trust, London, United Kingdom 

Corresponding authors: Clare M. Lloyd, PhD, National Heart and Lung Institute, Faculty of Medicine, Dr Victor Phillip Dahdaleh Building, Imperial College London, Du Cane Road, London W12 0NN. National Heart and Lung Institute Faculty of Medicine Imperial College London London United Kingdom ∗∗ Franz Puttur, PhD, National Heart and Lung Institute, Faculty of Medicine, Imperial College London, Dr Victor Phillip Dahdaleh Building, level 3, office 320, Imperial College Hammersmith Campus, Du Cane Road, London W12 0NN, UK. National Heart and Lung Institute Faculty of Medicine Imperial College London Dr Victor Phillip Dahdaleh Building level 3 office 320 Imperial College Hammersmith Campus, Du Cane Road London W12 0NN UK

Graphical abstract




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Abstract

Background

Airway remodeling is a prominent pathologic feature in preschool wheeze (PSW) and school-age asthma (SA). Although the relationships between altered lung function, extracellular matrix (ECM) changes, and airway remodeling are described in PSW and SA, the underlying mechanisms remain undefined.

Objective

We sought to investigate mechanisms resulting in altered airway ECM landscape in PSW (1-5 years of age) and SA (6-16 years of age) and track ECM dynamics in house dust mite (HDM)–exposed neonatal mice.

Methods

We applied spatial transcriptomics, confocal microscopy, and SHG microscopy in PSW and SA endobronchial biopsy specimens and in HDM-exposed neonatal mice lung specimens to reveal transcriptional, phenotypic, and structural ECM–associated changes during allergic airway inflammation.

Results

Spatial transcriptomic analysis of the airways of children with PSW and SA revealed increased gene expression for fibrillar collagens I, II, and III and basement membrane collagen VI in fibroblast-rich regions in both diseases. Similarly, increased collagen III and collagen VI deposition with exaggerated collagen fibril disorganization was observed in the peribronchial regions of HDM-exposed neonatal mice. Collagen disorganization was also evident in the airways of children with PSW and SA and was accompanied by increased production of bronchial epithelial cell–derived lumican and increased airway lumican in children with PSW, children with SA, and HDM-exposed neonatal mice. Lumican directly altered primary healthy airway fibroblast function, increasing proliferation and collagen production.

Conclusions

We demonstrate a previously uncharacterized role of collagen-associated phenotypic and geometric changes in early-life airway remodeling and show lumican as a crucial remodeling factor associated with collagen organization in PSW and SA.

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Key words : Preschool wheeze, school-age asthma, early life immunity, extracellular matrix

Abbreviations used : AAD, AHR, ASM, BAL, BEC, ECM, FGF, FGFR, GLCM, HDM, HH, HLF, IDM, PCLS, PDGF, PSW, RBM, RI, SA, SHG


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Vol 157 - N° 1

P. 176-189 - janvier 2026 Regresar al número
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