Coenzyme Q10 deficiency can be expected to compromise Sirt1 activity.
James J Di NicolantonioMark F McCartyJames H O'KeefePublished in: Open heart (2022)
For reasons that remain unclear, endogenous synthesis and tissue levels of coenzyme Q10 (CoQ10) tend to decline with increasing age in at least some tissues. When CoQ10 levels are sufficiently low, this compromises the efficiency of the mitochondrial electron transport chain, such that production of superoxide by site 2 increases and the rate of adenosine triphosphate production declines. Moreover, CoQ10 deficiency can be expected to decrease activities of Sirt1 and Sirt3 deacetylases, believed to be key determinants of health span. Reduction of the cytoplasmic and mitochondrial NAD + /NADH ratio consequent to CoQ10 deficit can be expected to decrease the activity of these deacetylases by lessening availability of their obligate substrate NAD + The increased oxidant production induced by CoQ10 deficiency can decrease the stability of Sirt1 protein by complementary mechanisms. And CoQ10 deficiency has also been found to lower mRNA expression of Sirt1. An analysis of the roles of Sirt1/Sirt3 in modulation of cellular function helps to rationalise clinical benefits of CoQ10 supplementation reported in heart failure, hypertension, non-alcoholic fatty liver disease, metabolic syndrome and periodontal disease. Hence, correction of CoQ10 deficiency joins a growing list of measures that have potential for amplifying health protective Sirt1/Sirt3 activities.
Keyphrases
- oxidative stress
- ischemia reperfusion injury
- heart failure
- metabolic syndrome
- healthcare
- public health
- mental health
- blood pressure
- type diabetes
- hydrogen peroxide
- cardiovascular disease
- insulin resistance
- risk assessment
- human health
- atrial fibrillation
- uric acid
- binding protein
- amino acid
- anti inflammatory
- liver fibrosis