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Metabolomic Profiles Differentiate Scleroderma-PAH From Idiopathic PAH and Correspond With Worsened Functional Capacity

Authors :
Mona Alotaibi
Junzhe Shao
Michael W. Pauciulo
William C. Nichols
Anna R. Hemnes
Atul Malhotra
Nick H. Kim
Jason X.-J. Yuan
Timothy Fernandes
Kim M. Kerr
Laith Alshawabkeh
Ankit A. Desai
Andreea M. Bujor
Robert Lafyatis
Jeramie D. Watrous
Tao Long
Susan Cheng
Stephen Y. Chan
Mohit Jain
Source :
Chest.
Publication Year :
2022

Abstract

The prognosis and therapeutic responses are worse for pulmonary arterial hypertension associated with systemic sclerosis (SSc-PAH) compared with idiopathic pulmonary arterial hypertension (IPAH). This discrepancy could be driven by divergence in underlying metabolic determinants of disease.Are circulating bioactive metabolites differentially altered in SSc-PAH vs IPAH, and can this alteration explain clinical disparity between these PAH subgroups?Plasma biosamples from 400 patients with SSc-PAH and 1,082 patients with IPAH were included in the study. Another cohort of 100 patients with scleroderma with no PH and 44 patients with scleroderma with PH was included for external validation. More than 700 bioactive lipid metabolites, representing a range of vasoactive and immune-inflammatory pathways, were assayed in plasma samples from independent discovery and validation cohorts using liquid chromatography/high-resolution mass spectrometry-based approaches. Regression analyses were used to identify metabolites that exhibited differential levels between SSc-PAH and IPAH and associated with disease severity.From hundreds of circulating bioactive lipid molecules, five metabolites were found to distinguish between SSc-PAH and IPAH, as well as associate with markers of disease severity. Relative to IPAH, patients with SSc-PAH carried increased levels of fatty acid metabolites, including lignoceric acid and nervonic acid, as well as eicosanoids/oxylipins and sex hormone metabolites.Patients with SSc-PAH are characterized by an unfavorable bioactive metabolic profile that may explain the poor and limited response to therapy. These data provide important metabolic insights into the molecular heterogeneity underlying differences between subgroups of PAH.

Details

ISSN :
19313543
Database :
OpenAIRE
Journal :
Chest
Accession number :
edsair.doi.dedup.....01d3f90f13a4cfb627344e035d105bf2