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. 2025 Oct;211(10):1823-1834.
doi: 10.1164/rccm.202502-0419OC.

Active Antigen-Specific Adaptive Immune Responses Are Shared among Patients with Progressive Fibrotic Interstitial Lung Disease

Tania E Velez  1 Young Me Yoon  2 Vaibhav Upadhyay  3 Sara E Vazquez  4 Cathryn T Lee  5 Kavitha C Selvan  5 Christopher S Law  3 Kelly M Blaine  5 Maile K Hollinger  1   2 Donna M Decker  5 Grace C Bingham  6 Christopher F Pastore  1 Catherine A Bonham  1 Marcus R Clark  7 Nathan R Schoettler  5 Mary E Strek  5 Robert D Guzy  8 Ayodeji Adegunsoye  5 Imre Noth  1 Paul J Wolters  3 Thomas H Barker  6 Mark S Anderson  3 Joseph L DeRisi  4 Anthony K Shum  3 Anne I Sperling  1   2
Affiliations

Active Antigen-Specific Adaptive Immune Responses Are Shared among Patients with Progressive Fibrotic Interstitial Lung Disease

Tania E Velez et al. Am J Respir Crit Care Med. 2025 Oct.

Abstract

Rationale: Enlargement of lung-associated lymph nodes (LNs) predicts worse survival in all patients with interstitial lung disease (ILD). This phenomenon occurs in both connective tissue disease-associated ILD and, surprisingly, idiopathic pulmonary fibrosis (IPF), where immune-driven pathogenesis is controversial. Objectives: To determine whether immune responses in the lung LNs of patients with ILD are antigen-specific and significant to pathology and etiology. Methods: ILD lung LNs excised at transplant (30 IPF, 7 interstitial pneumonia with autoimmune features, 4 hypersensitivity pneumonitis, 5 connective tissue disease-associated ILD, 5 other ILD) and 36 donor control lung LNs were analyzed by spectral flow cytometry. Formalin-fixed lung LNs and OCT-fixed lung samples of patients with IPF were used to determine germinal center (GC) and antigen-specific responses. Serum autoantibody responses were measured by radioligand binding assay. Measurements and Main Results: All patients with ILD revealed a common adaptive immune landscape of antigen responses in lung LNs characterized by the presence of GC B cells, T follicular helper cells, and activated T cells. Immunological synapses identified in the lung LNs demonstrated that antigen stimulation is ongoing in patients with ILD. Lung LN frequencies of T follicular helper and T regulatory cells correlated with circulating antibody concentrations to ABLIM1, a recently identified autoantigen expressed widely, including in aberrant basaloid cells that are uniquely found in fibrotic lungs. Conclusions: Antigen-induced activation and development of GC in enlarged lung LNs represents a shared immunopathologic mechanism associated with progressive pulmonary fibrosis among patients with ILD, regardless of etiology. Autoantigens overexpressed in progressive pulmonary fibrosis may be key drivers of these GC responses.

Keywords: adaptive immunity; germinal centers; interstitial lung disease; lymph nodes; pulmonary fibrosis.

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