Metabolomic Profiling of Left Ventricular Diastolic Dysfunction in Women With or at Risk for HIV Infection: The Women's Interagency HIV Study

Author:

Bravo Claudio A.1,Hua Simin2,Deik Amy3,Lazar Jason4,Hanna David B.2,Scott Justin3,Chai Jin Choul2,Kaplan Robert C.25,Anastos Kathryn26,Robles Octavio A.7,Clish Clary B.3,Kizer Jorge R.8,Qi Qibin2

Affiliation:

1. Division of Cardiology Department of Medicine Columbia University Medical Center New York NY

2. Department of Epidemiology & Population Health Albert Einstein College of Medicine Bronx NY

3. Metabolomics Platform Broad Institute of MIT and Harvard Cambridge MA

4. Division of Cardiovascular Medicine State University of New York Downstate Medical Center Brooklyn NY

5. Public Health Sciences Division Fred Hutchinson Cancer Research Center Seattle WA

6. Department of Medicine Albert Einstein College of Medicine Bronx NY

7. Department of Biologic Sciences Universidad de Chile Santiago Chile

8. Division of Cardiology San Francisco Veterans Affairs Health Care System University of California San Francisco San Francisco CA

Abstract

Background People living with HIV have an increased risk of left ventricular diastolic dysfunction ( LVDD ) and heart failure. HIV ‐associated LVDD may reflect both cardiomyocyte and systemic metabolic derangements, but the underlying pathways remain unclear. Methods and Results To explore such pathways, we conducted a pilot study in the Bronx and Brooklyn sites of the WIHS (Women's Interagency HIV Study) who participated in concurrent, but separate, metabolomics and echocardiographic ancillary studies. Liquid chromatography tandem mass spectrometry–based metabolomic profiling was performed on plasma samples from 125 HIV‐infected (43 with LVDD) and 35 HIV‐uninfected women (9 with LVDD). Partial least squares discriminant analysis identified polar metabolites and lipids in the glycerophospholipid‐metabolism and fatty‐acid‐oxidation pathways associated with LVDD . After multivariable adjustment, LVDD was significantly associated with higher concentrations of diacylglycerol 30:0 (odds ratio [ OR ], 1.60, 95% CI [1.01–2.55]); triacylglycerols 46:0 ( OR 1.60 [1.04–2.48]), 48:0 ( OR 1.63 [1.04–2.54]), 48:1 ( OR 1.62 [1.01–2.60]), and 50:0 ( OR 1.61 [1.02–2.53]); acylcarnitine C7 ( OR 1.88 [1.21–2.92]), C9 ( OR 1.99 [1.27–3.13]), and C16 ( OR 1.80 [1.13–2.87]); as well as lower concentrations of phosphocholine ( OR 0.59 [0.38–0.91]). There was no evidence of effect modification of these relationships by HIV status. Conclusions In this pilot study, women with or at risk of HIV with LVDD showed alterations in plasma metabolites in the glycerophospholipid‐metabolism and fatty‐acid‐oxidation pathways. Although these findings require replication, they suggest that improved understanding of metabolic perturbations and their potential modification could offer new approaches to prevent cardiac dysfunction in this high‐risk group.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

Reference44 articles.

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