QMCVIVAPMar 10

Association of Radiologic PPFE Change with Mortality in Lung Cancer Screening Cohorts

arXiv:2603.09531v14.7h-index: 12
Predicted impact top 82% in QM · last 90 daysOriginality Synthesis-oriented
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This research addresses the unclear clinical significance of radiologic PPFE progression in lung cancer screening populations, providing a potential imaging biomarker for identifying individuals at increased respiratory risk, though it is incremental as it applies an existing method to new data.

The study investigated whether longitudinal change in pleuroparenchymal fibroelastosis (PPFE) quantified on low-dose CT scans associates with mortality and respiratory morbidity in lung cancer screening populations, finding that PPFE progression independently associated with mortality in two cohorts (NLST: HR 1.25; SUMMIT: HR 3.14) and with adverse clinical outcomes like higher respiratory admissions.

Background: Pleuroparenchymal fibroelastosis (PPFE) is an upper lobe predominant fibrotic lung abnormality associated with increased mortality in established interstitial lung disease. However, the clinical significance of radiologic PPFE progression in lung cancer screening populations remains unclear. We investigated whether longitudinal change in PPFE quantified on low dose CT independently associates with mortality and respiratory morbidity. Methods: We analysed longitudinal low-dose CT scans and clinical data from two lung cancer screening studies: the National Lung Screening Trial (NLST; n=7980) and the SUMMIT study (n=8561). An automated algorithm quantified PPFE volume on baseline and follow up scans. Annualised change in PPFE (dPPFE) was derived and dichotomised using a distribution based threshold to define progressive PPFE. Associations between dPPFE and mortality were evaluated using Cox proportional hazards models adjusted for demographic and clinical variables. In the SUMMIT cohort, dPPFE was also examined in relation to clinical outcomes. Findings: dPPFE independently associated with mortality in both cohorts (NLST: HR 1.25, 95% CI 1.01-1.56, p=0.042; SUMMIT: HR 3.14, 95% CI 1.66-5.97, p<0.001). Kaplan-Meier curves showed reduced survival among participants with progressive PPFE in both cohorts. In SUMMIT, dPPFE was associated with higher respiratory admissions (IRR 2.79, p<0.001), increased antibiotic and steroid use (IRR 1.55, p=0.010), and a trend towards higher mMRC scores (OR 1.40, p=0.055). Interpretation: Radiologic PPFE progression independently associates with mortality across two large lung cancer screening cohorts and with adverse clinical outcomes. Quantitative assessment of PPFE progression may provide a clinically relevant imaging biomarker for identifying individuals at increased respiratory risk within screening programmes.

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