What question did this study set out to answer?

This study aims to assess the independent relationship between eosinophilia levels and exacerbation frequency in COPD patients.

May 20, 2026

B44-23 Recounting the Risk: Serial Eosinophils and Exacerbations in COPD

Puntos clave

This study aims to assess the independent relationship between eosinophilia levels and exacerbation frequency in COPD patients.
Retrospective cohort analysis in São Paulo, Brazil (June 2022 - June 2025).
Patients were categorized based on eosinophil counts: any-time ≥300 cells/µL or always <300.
Negative binomial models analyzed exacerbation counts while adjusting for relevant covariates.
In the study, 33% of patients exhibited eosinophilia ≥300 cells/µL.
Unadjusted analysis showed higher exacerbation rates with eosinophilia (IRR 1.64, 95% CI 1.02-2.63, p=0.042).
After adjustments, the association diminished to IRR 1.31 (95% CI 0.87-1.96, p=0.190), with FEV1% predicted demonstrating a significant protective effect.

Resumen

Abstract Background Type 2 (T2) inflammation, identified by peripheral blood eosinophils, is a recognized therapeutic target in COPD. Pivotal trials (BOREAS, NOTUS, MATINEE) commonly apply ≥ 300 cells/µL to define an eosinophil-high phenotype. However, real-world evidence combining serial eosinophil assessment with explicit asthma exclusion remains limited. Objective To determine whether any-time eosinophilia ≥ 300 cells/µL (vs always 300 cells/µL) is independently associated with recent exacerbation burden. Methods Retrospective, single-center cohort (São Paulo, Brazil; June 2022-June 2025) based on outpatient electronic medical records. Peripheral blood eosinophils were extracted immediately after each dated entry, and patients were classified as any-time ≥300 or always 300. Individuals with any asthma-suggestive features (family/personal history, nocturnal worsening, seasonal pattern) were excluded. Exacerbations were counted only for 2023-2025. We performed (i) a negative binomial (NB) model without covariates to obtain the crude IRR (displayed in the figure), and (ii) a multivariable NB model (age, FEV1% predicted, inhaled corticosteroid ICS use, LAMA/LABA use) to estimate the adjusted IRR (ICS effect not interpreted due to indication bias). Complete-case analysis was used. Results N = 99 patients were included; median of 3 eosinophil measurements per patient (IQR 2-4). Any-time eosinophilia was present in 33/99 (33%). Unadjusted NB: eosinophils ≥300 were associated with higher exacerbation counts, IRR 1.64 (95% CI 1.02-2.63), p = 0.042. Adjusted NB: the association attenuated and was not statistically significant, IRR 1.31 (95% CI 0.87-1.96), p = 0.190. FEV1% predicted remained independently protective, IRR 0.98 per percentage point (95% CI 0.967-0.994), p = 0.005. Conclusions In an asthma-excluded Brazilian cohort with serial eosinophil measurements, a binary, trial-aligned definition of eosinophilia (≥300 cells/µL at any time) showed a significant crude association with exacerbation burden, which attenuated after adjustment; FEV1% was a robust inverse correlate. These data complement BOREAS, NOTUS and MATINEE, underscoring that serial phenotyping adds operational clarity for patient selection, while emphasizing the need for prospective studies with uniform follow-up and richer covariate control (e.g., smoking status, sex, recent systemic corticosteroids) to refine the exacerbation signal in T2-leaning COPD. This abstract is funded by: None

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B44-23 Recounting the Risk: Serial Eosinophils and Exacerbations in COPD

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