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The transcriptome of CD14+CD163-HLA-DRlow monocytes predicts mortality in Idiopathic Pulmonary Fibrosis.

Abstract

BACKGROUND: The association between immune-cell-specific transcriptomic profiles and mortality in IPF is unknown. METHODS: We profiled peripheral blood mononuclear cells (PBMC) by single-cell RNA sequencing (scRNA-seq) and investigated which immune-cell-specific transcriptomic profile predicted IPF outcomes consistently. Prognostic accuracy was investigated in PBMC, Bronchoalveolar Lavage (BAL) and lung tissue. Findings were validated by flow cytometry, analysis of independent scRNA-seq datasets and cellular deconvolution. We investigated the function of this transcriptomic profile and its cellular source in lung tissue (overall sample size:1054, IPF:555, other:499). Connectivity map and LASSO regression were used to identify drug candidates and a subset of genes with prognostic potential, respectively. RESULTS: A 230-gene-up-score (Pittsburgh-PBMC) from CD14+CD163-HLA-DRlow monocytes predicted mortality in Chicago PBMC cohort (HR: 6.58, 95%CI:2.15-20.13, p=0.001), in BAL pooled analysis (HR: 2.20, 95%CI: 1.44-3.37, p=0.0003) and negatively correlated with Forced Vital Capacity (FVC) in lung tissues (rho=-0.2, p=0.02). CD14+CD163-HLA-DRlow monocytes were higher in progressive versus stable IPF (12.59%, 95%CI:9.66-16.23, versus 7.61%, 95%CI:6.68-10.21, p=0.014). High risk IPF patients had decreased expression of T-cell co-stimulatory genes (Pittsburgh and Chicago p<0.01). CD14+HLA-DRlow monocytes had higher expression of profibrotic, proangiogenic and chemotactic factors compared to CD14+HLA-DRhi monocytes (p<0.05). The 230-gene-up-score correlated with the SPP1+fibrosis-associated macrophages-gene-score in lung tissues (rho=0.19, p<2.2e-16). Connectivity map identified drug categories to reverse the 230-gene-signature. A subset of six genes retained predictive performance (pooled PBMC cohorts -HR: 4.79, 95%CI:2.58-8.92, p<0.0001). CONCLUSIONS: The transcriptome of CD14+CD163-HLA-DRlow monocytes is associated with increased mortality in patients with IPF. Its reversal should be investigated as a precision-based therapy in IPF.

Authors: Karampitsakos T, Jia M, Tourki B, Fatima Z, Visinescu B, Perrot CY, Fadli T, Zhao A, Unterman A, Schneider MA, Bandyopadhyay D, Juan-Guardela BM, Vamvakaris I, Prasse A, Noth I, Liggett S, Kreuter M, Drake W, Tzouvelekis A, Garcia JGN, Herzog E, Kaminski
Journal: Eur Respir J. 2025 Dec 11:2500804. doi: 10.1183/13993003.00804-2025.
Year: 2025
PubMed: PMID: 41360505 (Go to PubMed)