Cluster analysis identifies novel real-world lung disease–pulmonary hypertension subphenotypes: implications for treatment response

Shelsey W. Johnson; Rui-Sheng Wang; Michael R. Winter; Kari R. Gillmeyer; Katarina Zeder; Elizabeth S. Klings; Ronald H. Goldstein; Renda Soylemez Wiener; Bradley A. Maron

doi:10.1183/23120541.00959-2023

ERJ Open Research (May 2024)

Cluster analysis identifies novel real-world lung disease–pulmonary hypertension subphenotypes: implications for treatment response

Shelsey W. Johnson,
Rui-Sheng Wang,
Michael R. Winter,
Kari R. Gillmeyer,
Katarina Zeder,
Elizabeth S. Klings,
Ronald H. Goldstein,
Renda Soylemez Wiener,
Bradley A. Maron

Affiliations

Shelsey W. Johnson: VA Boston Healthcare System, Boston, MA, USA
Rui-Sheng Wang: Department of Medicine, Brigham and Women's Hospital, Boston, MA, USA
Michael R. Winter: Boston University School of Public Health, Biostatistics and Epidemiology Data Analytics Center, Boston, MA, USA
Kari R. Gillmeyer: VA Boston Healthcare System, Boston, MA, USA
Katarina Zeder: Department of Medicine, University of Maryland School of Medicine, Baltimore, MD, USA
Elizabeth S. Klings: The Pulmonary Center, Division of Pulmonary, Allergy, Sleep and Critical Care, and Boston University School of Medicine, Boston, MA, USA
Ronald H. Goldstein: VA Boston Healthcare System, Boston, MA, USA
Renda Soylemez Wiener: VA Boston Healthcare System, Boston, MA, USA
Bradley A. Maron: VA Boston Healthcare System, Boston, MA, USA

DOI: https://doi.org/10.1183/23120541.00959-2023
Journal volume & issue: Vol. 10, no. 3

Abstract

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Background Clinical trials repurposing pulmonary arterial hypertension (PAH) therapies to patients with lung disease- or hypoxia-pulmonary hypertension (PH) (classified as World Health Organization Group 3 PH) have failed to show a consistent benefit. However, Group 3 PH clinical heterogeneity suggests robust phenotyping may inform detection of treatment-responsive subgroups. We hypothesised that cluster analysis would identify subphenotypes with differential responses to oral PAH therapy. Methods Two k-means analyses were performed on a national cohort of US veterans with Group 3 PH; an inclusive model (I) of all treated patients (n=196) and a haemodynamic model (H) limited to patients with right heart catheterisations (n=112). The primary outcome was organ failure or all-cause mortality by cluster. An exploratory analysis evaluated within-cluster treatment effects. Results Three distinct clusters of Group 3 PH patients were identified. In the inclusive model (C1I n=43, 21.9%; C2I n=102, 52.0%; C3I n=51, 26.0%), lung disease and spirometry drove cluster assignment. By contrast, in the haemodynamic model (C1H n=44, 39.3%; C2H n=43, 38.4%; C3H n=25, 22.3%), right heart catheterisation data surpassed the importance of lung disease and spirometry. In the haemodynamic model, compared to C3H, C1H experienced the greatest hazard for respiratory failure or death (HR 6.1, 95% CI 3.2–11.8). In an exploratory analysis, cluster determined treatment response (p=0.006). Conclusions regarding within-cluster treatment responses were limited by significant differences between select variables in the treated and untreated groups. Conclusions Cluster analysis identifies novel real-world subphenotypes of Group 3 PH patients with distinct clinical trajectories. Future studies may consider this methodological approach to identify subgroups of heterogeneous patients that may be responsive to existing pulmonary vasodilatory therapies.

Published in ERJ Open Research

ISSN: 2312-0541 (Online)
Publisher: European Respiratory Society
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://openres.ersjournals.com/

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