Polymorphic variants at NDUFC2, encoding a mitochondrial complex I subunit, associate with cardiac hypertrophy in human hypertension

Giovanna Gallo; Maurizio Forte; Maria Cotugno; Simona Marchitti; Rosita Stanzione; Giuliano Tocci; Franca Bianchi; Silvia Palmerio; Mariarosaria Scioli; Giacomo Frati; Sebastiano Sciarretta; Emanuele Barbato; Massimo Volpe; Speranza Rubattu

doi:10.1186/s10020-023-00701-x

Polymorphic variants at NDUFC2, encoding a mitochondrial complex I subunit, associate with cardiac hypertrophy in human hypertension

Mol Med. 2023 Aug 9;29(1):107. doi: 10.1186/s10020-023-00701-x.

Authors

Giovanna Gallo^#¹, Maurizio Forte^#², Maria Cotugno², Simona Marchitti², Rosita Stanzione², Giuliano Tocci¹, Franca Bianchi², Silvia Palmerio³, Mariarosaria Scioli², Giacomo Frati^{2

4}, Sebastiano Sciarretta^{2

4}, Emanuele Barbato¹, Massimo Volpe^{1

5}, Speranza Rubattu^{6

7}

Affiliations

¹ Department of Clinical and Molecular Medicine, School of Medicine and Psychology, Sapienza University, Rome, Italy.
² IRCCS Neuromed, Pozzilli (Is), Italy.
³ Department of Medicine, University of Verona School of Medicine, Verona University Hospital Trust, Verona, Italy.
⁴ Department of Medical-Surgical Sciences and Biotechnologies, Sapienza University of Rome, Latina, Italy.
⁵ IRCCS S. Raffaele, Rome, Italy.
⁶ Department of Clinical and Molecular Medicine, School of Medicine and Psychology, Sapienza University, Rome, Italy. speranzadonatella.rubattu@uniroma1.it.
⁷ IRCCS Neuromed, Pozzilli (Is), Italy. speranzadonatella.rubattu@uniroma1.it.

^# Contributed equally.

Abstract

Background: A dysfunction of NADH dehydrogenase, the mitochondrial Complex I (CI), associated with the development of left ventricular hypertrophy (LVH) in previous experimental studies. A deficiency of Ndufc2 (subunit of CI) impairs CI activity causing severe mitochondrial dysfunction. The T allele at NDUFC2/rs11237379 variant associates with reduced gene expression and impaired mitochondrial function. The present study tested the association of both NDUFC2/rs11237379 and NDUFC2/rs641836 variants with LVH in hypertensive patients. In vitro studies explored the impact of reduced Ndufc2 expression in isolated cardiomyocytes.

Methods: Two-hundred-forty-six subjects (147 male, 59.7%), with a mean age of 59 ± 15 years, were included for the genetic association analysis. Ndufc2 silencing was performed in both H9c2 and rat primary cardiomyocytes to explore the hypertrophy development and the underlying signaling pathway.

Results: The TT genotype at NDUFC2/rs11237379 associated with significantly reduced gene expression. Multivariate analysis revealed that patients carrying this genotype showed significant differences for septal thickness (p = 0.07), posterior wall thickness (p = 0.008), RWT (p = 0.021), LV mass/BSA (p = 0.03), compared to subjects carrying either CC or CT genotypes. Patients carrying the A allele at NDUFC2/rs641836 showed significant differences for septal thickness (p = 0.017), posterior wall thickness (p = 0.011), LV mass (p = 0.003), LV mass/BSA (p = 0.002) and LV mass/height^2.7(p = 0.010) after adjustment for covariates. In-vitro, the Ndufc2 deficiency-dependent mitochondrial dysfunction caused cardiomyocyte hypertrophy, pointing to SIRT3-AMPK-AKT-MnSOD as a major underlying signaling pathway.

Conclusions: We demonstrated for the first time a significant association of NDUFC2 variants with LVH in human hypertension and highlight a key role of Ndufc2 deficiency-dependent CI mitochondrial dysfunction on increased susceptibility to cardiac hypertrophy development.

Keywords: Cardiac hypertrophy; Hypertension; Mitochondrial complex I; Mitochondrial dysfunction; NDUFC2; SIRT3.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Animals
Cardiomegaly* / genetics
Electron Transport Complex I / genetics
Genotype
Humans
Hypertension* / complications
Hypertension* / genetics
Hypertrophy, Left Ventricular / complications
Hypertrophy, Left Ventricular / genetics
Male
Middle Aged
Rats
Signal Transduction

Substances

NDUFC2 protein, human
Electron Transport Complex I