Whole blood mitochondrial copy number in clinical populations with mood disorders: a meta-analysis

Calarco, Cali A.; Keppetipola, Swarnapali M.; Kumar, Gautam; Shipper, Andrea G.; Lobo, Mary Kay

doi:10.1101/2023.09.13.557572

2023

DOI: 10.1101/2023.09.13.557572

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Whole blood mitochondrial copy number in clinical populations with mood disorders: a meta-analysis

Cali A. Calarco,

Swarnapali M. Keppetipola,

Gautam Kumar

et al.

Abstract: Background: Major depressive disorder (MDD) and bipolar disorder (BD), are globally prevalent, contributing to significant disease burden and adverse health outcomes. These mood disorders are associated with changes in many aspects of brain reward pathways, yet cellular and molecular changes in the brain are not readily available in clinical populations. Therefore, the use of biomarkers as proxies for changes in the brain are necessary. The proliferation of mitochondria in blood has emerged as a potentially us… Show more

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Cited by 2 publications

References 81 publications

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Mitochondria at the crossroad of dysregulated inflammatory and metabolic processes in bipolar disorders

Bernard,

Tamouza,

Godin

et al. 2025

Brain, Behavior, and Immunity

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Mitochondria at the crossroad of dysregulated inflammatory and metabolic processes in bipolar disorders

Bernard,

Tamouza,

Godin

et al. 2025

Brain, Behavior, and Immunity

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Does BioAge identify accelerated aging in individuals with bipolar disorder? An exploratory study in the FACE‐BD cohort

Etain,

Marie‐Claire,

Spano

et al. 2024

Bipolar Disorders

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BackgroundIndividuals with bipolar disorders (BD) have an estimated loss of life expectancy around 10–15 years. Several laboratory‐measured biomarkers of accelerated aging exist (e.g., telomere length), however with a questionable transferability to bedside. There is a need for easily and inexpensively measurable markers of aging, usable in routine practice, such as BioAge.MethodsWe calculated BioAge that estimates biological age based on routine blood tests and a physical exam, in a sample of 2220 outpatients with BD. We investigated associations between BioAge Acceleration (BioAgeAccel), which is an indicator of accelerated aging, and sociodemographic variables, clinical variables, and current psychotropic medication use.ResultsMean chronological age was 40.2 (±12.9). Mean BioAge was 39.1 (±12.4). Mean BioAgeAccel was 0.08 (±1.8). A minority of individuals (15%) had a BioAgeAccel above 2 years. Multivariable analyses suggested strong associations between a higher BioAgeAccel and younger age, male sex, overweight and sleep disturbances. Regarding current psychotropic medication use, discrepancies between univariate and multivariate analyses were observed.ConclusionsA minority of individuals with BD had an accelerated aging as measured by BioAge. We identified associations with potentially modifiable factors, such as higher body mass index and sleep disturbances, that are however nonspecific to BD. These results require replications in independent samples of individuals with BD, and comparisons with a control group matched for age and gender. Longitudinal studies are also required to test whether any change in metabolic health, or sleep might decrease BioAgeAccel.

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Whole blood mitochondrial copy number in clinical populations with mood disorders: a meta-analysis

Cited by 2 publications

References 81 publications

Mitochondria at the crossroad of dysregulated inflammatory and metabolic processes in bipolar disorders

Mitochondria at the crossroad of dysregulated inflammatory and metabolic processes in bipolar disorders

Does BioAge identify accelerated aging in individuals with bipolar disorder? An exploratory study in the FACE‐BD cohort

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