Molecular Features and Stages of Pulmonary Fibrosis Driven by Type 2 Inflammation

Hamid Mattoo; Dinesh S Bangari; Sheila Cummings; Zachary Humulock; David Habiel; Ethan Y Xu; Nathan Pate; Robert Resnick; Virginia Savova; George Qian; Christian Beil; Ercole Rao; Frank O Nestle; Paul J Bryce; Arun Subramaniam

doi:10.1165/rcmb.2022-0301OC

Molecular Features and Stages of Pulmonary Fibrosis Driven by Type 2 Inflammation

Am J Respir Cell Mol Biol. 2023 Oct;69(4):404-421. doi: 10.1165/rcmb.2022-0301OC.

Authors

Affiliations

¹ Precision Medicine and Computational Biology.
² Discovery Pathology, Translational In Vivo Models Platform, and.
³ Immunology and Inflammation Research Therapeutic Area.
⁴ Aspen Neuroscience, San Diego, California.
⁵ Biologics Research, Sanofi, Frankfurt, Germany; and.
⁶ US Medical Affairs, Sanofi, Cambridge, Massachusetts.

PMID: 37369139
DOI: 10.1165/rcmb.2022-0301OC

Abstract

Systemic sclerosis (SSc) is a progressive, multiorgan disease with limited treatment options. Although a recent proof-of-concept study using romilkimab or SAR156597, a bispecific IL-4/IL-13 antibody, suggests a direct role of these cytokines in the pathophysiology of SSc, their contributions to the balance between inflammation and fibrosis are unclear. Here, we determine the roles of type 2 inflammation in fibrogenesis using FRA2-Tg (Fos-related antigen 2-overexpressing transgenic) mice, which develop spontaneous, age-dependent progressive lung fibrosis. We defined the molecular signatures of inflammation and fibrosis at three key stages in disease progression, corresponding to preonset, inflammatory dominant, and fibrosis dominant biology, and revealed an early increase in cytokine-cytokine receptor interactions and antigen-processing and presentation pathways followed by enhanced Th2- and M2 macrophage-driven type 2 responses. This type 2 inflammation progressed to extensive fibrotic pathology by 14-18 weeks of age, with these gene signatures overlapping significantly with those seen in the lungs of patients with SSc with interstitial lung disease (ILD). These changes were also evident in the histopathology, which showed perivascular and peribronchiolar inflammation with prominent eosinophilia and accumulation of profibrotic M2-like macrophages followed by rapid progression to fibrosis with thickened alveolar walls with multifocal fibrotic bands and signs of interstitial pneumonia. Critically, treatment with a bispecific antibody targeting IL-4 and IL-13 during the inflammatory phase abrogated the Th2 and M2 responses and led to near-complete abrogation of lung fibrosis. These data recapitulate important features of fibrotic progression in the lungs of patients with SSc-ILD and enhance our understanding of the progressive pathobiology of SSc. This study also further establishes FRA2-Tg mice as a valuable tool for testing future therapeutic agents in SSc-ILD.

Keywords: IL-13; IL-4; fibrosis; interstitial lung disease; systemic sclerosis.

MeSH terms

Animals
Cytokines
Fibrosis
Humans
Inflammation / pathology
Interleukin-13
Interleukin-4
Lung / pathology
Lung Diseases, Interstitial* / pathology
Mice
Mice, Transgenic
Pulmonary Fibrosis* / pathology
Scleroderma, Systemic*

Substances

Interleukin-13
Interleukin-4
Cytokines