Methylated Arginine Metabolites as Biomarkers for Clinical Status and Response to Type 5 Phosphodiesterase Inhibition in Patients With Fontan Circulation

Ari Cedars; Cedric Manlhiot; Bhargava Kumar Chinni; Alexander R. Opotowsky; Kristian Becker; Anne Le; Pratik Khare; Jong Love Ko; Allen Everett; Shelby Kutty; Mark W. Russell; R. Mark Payne; Andrew M. Atz; Brian W. McCrindle; Rahul H. Rathod; Matthew Lewis; David Goldberg; Kevin Hill; Michelle Ploutz; Jon Detterich; Kurt Schumacher; Robert Whitehill; Daniel J. Penny; Mark Cartoski; Rachel Sullivan; Matthew Files; Ruchira Garg; Jonathan Wagner; Roni Jacobsen; Todd Nowlen; Scott Fletcher; Jennifer Conway; Gi Boem Kim; Fred Wu; Victor Zak

doi:10.1161/jaha.124.038061

Journal of the American Heart Association: Cardiovascular and Cerebrovascular Disease (Apr 2025)

Methylated Arginine Metabolites as Biomarkers for Clinical Status and Response to Type 5 Phosphodiesterase Inhibition in Patients With Fontan Circulation

Ari Cedars,
Cedric Manlhiot,
Bhargava Kumar Chinni,
Alexander R. Opotowsky,
Kristian Becker,
Anne Le,
Pratik Khare,
Jong Love Ko,
Allen Everett,
Shelby Kutty,
Mark W. Russell,
R. Mark Payne,
Andrew M. Atz,
Brian W. McCrindle,
Rahul H. Rathod,
Matthew Lewis,
David Goldberg,
Kevin Hill,
Michelle Ploutz,
Jon Detterich,
Kurt Schumacher,
Robert Whitehill,
Daniel J. Penny,
Mark Cartoski,
Rachel Sullivan,
Matthew Files,
Ruchira Garg,
Jonathan Wagner,
Roni Jacobsen,
Todd Nowlen,
Scott Fletcher,
Jennifer Conway,
Gi Boem Kim,
Fred Wu,
Victor Zak

Affiliations

Ari Cedars: Johns Hopkins University Baltimore MD USA
Cedric Manlhiot: Johns Hopkins University Baltimore MD USA
Bhargava Kumar Chinni: Johns Hopkins University Baltimore MD USA
Alexander R. Opotowsky: Cincinnati Children’s Hospital University of Cincinnati College of Medicine Cincinnati OH USA
Kristian Becker: Cincinnati Children’s Hospital University of Cincinnati College of Medicine Cincinnati OH USA
Anne Le: Gigantest Inc. Baltimore MD USA
Pratik Khare: Johns Hopkins University Baltimore MD USA
Jong Love Ko: Johns Hopkins University Baltimore MD USA
Allen Everett: Johns Hopkins University Baltimore MD USA
Shelby Kutty: Johns Hopkins University Baltimore MD USA
Mark W. Russell: C.S. Mott Children’s Hospital University of Michigan Ann Arbor MI USA
R. Mark Payne: Riley Hospital for Children Indianapolis IN USA
Andrew M. Atz: Department of Pediatrics Medical University of South Carolina Charlotte SC USA
Brian W. McCrindle: Labatt Family Heart Centre The Hospital for Sick Children, University of Toronto ON Canada
Rahul H. Rathod: Boston Children’s Hospital Boston MA USA
Matthew Lewis: Columbia University New York NY USA
David Goldberg: Children’s Hospital of Philadelphia Philadelphia PA USA
Kevin Hill: Duke University Medical Center Durham NC USA
Michelle Ploutz: University of Utah Salt Lake City UT USA
Jon Detterich: Children’s Hospital Los Angeles Los Angeles CA USA
Kurt Schumacher: C.S. Mott Children’s Hospital University of Michigan Ann Arbor MI USA
Robert Whitehill: Children’s Healthcare of Atlanta Atlanta GA USA
Daniel J. Penny: Texas Children’s Hospital Houston TX USA
Mark Cartoski: Nemours Childrens Health Wilmington DE USA
Rachel Sullivan: Monroe Carrell Jr. Children’s Hospital at Vanderbilt University Nashville TN USA
Matthew Files: Seattle Children’s Hospital Seattle WA USA
Ruchira Garg: Cedars‐Sinai Medical Center Los Angeles CA USA
Jonathan Wagner: Children’s Mercy Kansas City Kansas City MO USA
Roni Jacobsen: Children’s Hospital of Colorado Denver CO USA
Todd Nowlen: Phoenix Children’s Hospital Phoenix AZ USA
Scott Fletcher: Children’s Nebraska Omaha NE USA
Jennifer Conway: Stollery Children’s Hospital Edmonton AB Canada
Gi Boem Kim: Seoul National University Hospital Seoul South Korea
Fred Wu: Boston Children’s Hospital Boston MA USA
Victor Zak: Carelon Research Newton MA USA

DOI: https://doi.org/10.1161/jaha.124.038061
Journal volume & issue: Vol. 14, no. 7

Abstract

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Background There is significant interest in NO pathway modulators, specifically type 5 phosphodiesterase inhibitors (PDE5is), to treat patients with a Fontan circulation. Trials, however, have had mixed results. The relationship between the NO pathway and clinical status in patients with Fontan circulation is a significant knowledge gap. Methods and Results We performed targeted metabolomic analysis using liquid chromatography coupled to mass spectrometry to quantify plasma NO pathway metabolite concentrations from 2 well‐characterized populations of patients with Fontan circulation: the Boston Adult Congenital Heart Disease Biobank and Fontan Udenafil Exercise Longitudinal studies. We investigated associations between NO metabolite concentrations and clinical outcomes, exercise capacity, and response to PDE5is. Increased plasma concentration of asymmetric dimethyl arginine (ADMA), an inhibitor of NO production, was associated with risk for hospitalization or death. Increased ADMA and symmetric dimethyl arginine (another inhibitor of NO production) concentrations were associated with decreased baseline exercise capacity among patients with Fontan circulation with <90% predicted peak oxygen uptake, and change in ADMA and symmetric dimethyl arginine concentrations were predictive of change in exercise capacity over time. Treatment with the PDE5i udenafil uncoupled this association. Finally, baseline ADMA and symmetric dimethyl arginine concentrations predicted response to PDE5is among patients with subnormal peak oxygen uptake. Conclusions Plasma concentrations of metabolites that inhibit NO flux are associated with negative clinical outcomes and worse exercise capacity. Moreover, metabolite shifts over time associated with increased NO flux are associated with improved exercise capacity. In patients with a Fontan circulation, the NO pathway modulators ADMA and symmetric dimethyl arginine may be useful as biomarkers of clinical status and predictive of response to PDE5is.

Published in Journal of the American Heart Association: Cardiovascular and Cerebrovascular Disease

ISSN: 2047-9980 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the circulatory (Cardiovascular) system
Website: https://www.ahajournals.org/journal/jaha

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