Instability in NAD+ metabolism leads to impaired cardiac mitochondrial function and communication

Knut H Lauritzen; Maria Belland Olsen; Mohammed Shakil Ahmed; Kuan Yang; Johanne Egge Rinholm; Linda H Bergersen; Qin Ying Esbensen; Lars Jansen Sverkeli; Mathias Ziegler; Håvard Attramadal; Bente Halvorsen; Pål Aukrust; Arne Yndestad

doi:10.7554/eLife.59828

Instability in NAD⁺ metabolism leads to impaired cardiac mitochondrial function and communication

Elife. 2021 Aug 3:10:e59828. doi: 10.7554/eLife.59828.

Authors

Knut H Lauritzen¹, Maria Belland Olsen¹, Mohammed Shakil Ahmed², Kuan Yang¹, Johanne Egge Rinholm³, Linda H Bergersen^{4

5}, Qin Ying Esbensen⁶, Lars Jansen Sverkeli⁷, Mathias Ziegler⁷, Håvard Attramadal², Bente Halvorsen^{1

8}, Pål Aukrust^{1

8

9}, Arne Yndestad^{1

8}

Affiliations

¹ Research Institute of Internal Medicine, Oslo University Hospital, Rikshospitalet and University of Oslo, Oslo, Norway.
² Institute for Surgical Research, Oslo University Hospital and University of Oslo, Oslo, Norway.
³ Department of Microbiology, Oslo University Hospital, Oslo, Norway.
⁴ Department of Oral Biology, University of Oslo, Oslo, Norway.
⁵ Department of Neuroscience and Pharmacology, Center for Healthy Aging, University of Copenhagen, Copenhagen, Denmark.
⁶ Department of Clinical Molecular Biology, University of Oslo and Akershus University Hospital, Nordbyhagen, Norway.
⁷ Department of Biomedicine, University of Bergen, Bergen, Norway.
⁸ Institute of Clinical Medicine, University of Oslo, Faculty of Medicine, Oslo, Norway.
⁹ Section of Clinical Immunology and Infectious Diseases, Oslo University Hospital Rikshospitalet, Oslo, Norway.

Abstract

Poly(ADP-ribose) polymerase (PARP) enzymes initiate (mt)DNA repair mechanisms and use nicotinamide adenine dinucleotide (NAD⁺) as energy source. Prolonged PARP activity can drain cellular NAD⁺ reserves, leading to de-regulation of important molecular processes. Here, we provide evidence of a pathophysiological mechanism that connects mtDNA damage to cardiac dysfunction via reduced NAD⁺ levels and loss of mitochondrial function and communication. Using a transgenic model, we demonstrate that high levels of mice cardiomyocyte mtDNA damage cause a reduction in NAD⁺ levels due to extreme DNA repair activity, causing impaired activation of NAD⁺-dependent SIRT3. In addition, we show that myocardial mtDNA damage in combination with high dosages of nicotinamideriboside (NR) causes an inhibition of sirtuin activity due to accumulation of nicotinamide (NAM), in addition to irregular cardiac mitochondrial morphology. Consequently, high doses of NR should be used with caution, especially when cardiomyopathic symptoms are caused by mitochondrial dysfunction and instability of mtDNA.

Keywords: DNA repair; NAD+; SIRT3; biochemistry; cardiovascular disease; chemical biology; human; mitochondrial dna; mouse; nicotinamide riboside.

Publication types

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

MeSH terms

Animals
DNA Damage
DNA Repair*
DNA, Mitochondrial / metabolism*
HeLa Cells
Heart / physiopathology*
Heart Diseases / physiopathology*
Humans
Mice
Mitochondria / metabolism
Myocardium / metabolism*
NAD / metabolism*
Niacinamide / adverse effects
Niacinamide / analogs & derivatives
Niacinamide / metabolism
Pyridinium Compounds / adverse effects
Sirtuins / antagonists & inhibitors

Substances

DNA, Mitochondrial
Pyridinium Compounds
nicotinamide-beta-riboside
NAD
Niacinamide
Sirtuins

Grants and funding

The funders had no role in study design, data collection and interpretation, or the decision to submit the work for publication.