Arginine-NO metabolites are associated with morbidity in single ventricle infants undergoing stage 2 palliation

Benjamin S Frank; Sierra Niemiec; Ludmila Khailova; Christopher A Mancuso; Tanner Lehmann; Max B Mitchell; Gareth J Morgan; Mark Twite; Michael V DiMaria; Jelena Klawitter; Jesse A Davidson

doi:10.1038/s41390-024-03162-y

Arginine-NO metabolites are associated with morbidity in single ventricle infants undergoing stage 2 palliation

Pediatr Res. 2024 Apr 2. doi: 10.1038/s41390-024-03162-y. Online ahead of print.

Affiliations

¹ University of Colorado Department of Pediatrics, Section of Cardiology, Denver, CO, USA. Benjamin.Frank@childrenscolorado.org.
² University of Colorado Department of Biostatistics and Informatics, Denver, CO, USA.
³ University of Colorado Department of Pediatrics, Section of Cardiology, Denver, CO, USA.
⁴ University of Colorado Department of Surgery, Denver, CO, USA.
⁵ University of Colorado Department of Anesthesiology, Denver, CO, USA.

PMID: 38565916
DOI: 10.1038/s41390-024-03162-y

Abstract

Background: Infants with single ventricle heart disease (SVHD) suffer morbidity from insufficient pulmonary blood flow, which may be related to impaired arginine metabolism. No prior study has reported quantitative mapping of arginine metabolites to evaluate the relationship between circulating metabolite levels and outcomes.

Methods: Prospective cohort study of 75 SVHD cases peri-Stage 2 and 50 healthy controls. We targeted pre- and post-op absolute serum quantification of 9 key members of the arginine metabolism pathway by tandem mass spectrometry. Primary outcomes were length of stay (LOS) and post-Stage 2 hypoxemia.

Results: Pre-op cases showed alteration in 6 metabolites including decreased arginine and increased asymmetric dimethyl arginine (ADMA) levels compared to controls. Post-op cases demonstrated decreased arginine and citrulline levels persisting through 48 h. Adjusting for clinical variables, lower pre-op and 2 h post-op concentrations of multiple metabolites, including arginine and citrulline, were associated with longer post-op LOS (p < 0.01). Increased ADMA at 24 h was associated with greater post-op hypoxemia burden (p < 0.05).

Conclusion: Arginine metabolism is impaired in interstage SVHD infants and is further deranged following Stage 2 palliation. Patients with greater metabolite alterations experience greater post-op morbidity. Decreased arginine metabolism may be an important driver of pathology in SVHD.

Impact: Interstage infants with SVHD have significantly altered arginine-nitric oxide metabolism compared to healthy children with deficiency of multiple pathway intermediates persisting through 48 h post-Stage 2 palliation. After controlling for clinical covariates and classic catheterization-derived predictors of Stage 2 readiness, both lower pre-operation and lower post-operation circulating metabolite levels were associated with longer post-Stage 2 LOS while increased post-Stage 2 ADMA concentration was associated with greater post-op hypoxemia. Arginine metabolism mapping offers potential for development using personalized medicine strategies as a biomarker of Stage 2 readiness and therapeutic target to improve pulmonary vascular health in infants with SVHD.

Arginine-NO metabolites are associated with morbidity in single ventricle infants undergoing stage 2 palliation

Authors

Affiliations

Abstract

Grants and funding