Blood-derived mitochondrial DNA copy number is associated with gene expression across multiple tissues and is predictive for incident neurodegenerative disease

Yang, Stephanie; Castellani, Christina A; Longchamps, Ryan J.; Pillalamarri, Vamsee; O’Rourke, Brian; Güallar, Eliseo; Arking, Dan E.

doi:10.1101/2020.07.17.209023

Cited by 15 publications

(18 citation statements)

References 76 publications

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“…chronic kidney disease 13 , heart failure 11 , and diabetes 75 ). Also consistent with this finding is recent work demonstrating that mtDNA-CN measured in blood is associated with mtRNA expression across numerous non-blood tissues, suggesting a link between mitochondrial function measured in blood and other tissues 76 .…”

Section: Discussionsupporting

confidence: 87%

“…We were able to identify a substantial proportion of the genes involved in mtDNA depletion syndromes (7/16, p = 3.09 × 10 −15 for enrichment), including TWNK, TFAM, DGUOK, MGME1, RRM2B, TYMP , and POLG . mtDNA depletion syndromes can be broken down into 5 subtypes based on their constellation of phenotypes 65 , and with the exception of cardiomyopathic subtypes (associated with mutations in AGK and SLC25A4 ), we were able to identify at least 1 gene from the other 4 subtypes, suggesting that our mtDNA-CN measurement in blood-derived DNA can identify genes widely relevant to non-blood phenotypes. This finding is consistent with a large body of work showing that mtDNA-CN measured in blood is associated with numerous aging-related phenotypes for which the primary tissue of interest is not blood (e.g.…”

Section: Discussionmentioning

confidence: 70%

“…Of particular interest, the GO term for amyloid beta is significantly enriched, reinforcing a link between mtDNA-CN and neurodegenerative disease [85][86][87] . Previous work from our lab using the UKB has shown that increased mtDNA-CN is associated with lower rates of prevalent neurodegenerative disease, and is predictive for decreased risk of incident neurodegenerative disease 76 . mtDNA-CN is also known to be decreased in the frontal cortex of Alzheimer's disease (AD) patients 88 .…”

Section: Discussionmentioning

confidence: 77%

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Genetic analysis of mitochondrial DNA copy number and associated traits identifies loci implicated in nucleotide metabolism, platelet activation, and megakaryocyte proliferation, and reveals a causal association of mitochondrial function with mortality

Longchamps

Yang

Castellani

et al. 2021

Preprint

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Blood-derived mitochondrial DNA copy number (mtDNA-CN) is a minimally invasive proxy measure of mitochondrial function that exhibits both inter-individual and intercellular variation. While mtDNA-CN has been previously associated with various aging-related diseases, little is known about the genetic factors that may modulate this phenotype. We performed a genome-wide association study (GWAS) in 465,809 individuals of White (European) ancestry from the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) consortium and the UK Biobank (UKB). We identified 129 SNPs with statistically significant, independent effects associated with mtDNA-CN across 96 loci. A combination of fine-mapping, variant annotation, co-localization, and gene set enrichment analyses were used to prioritize genes within each of the 129 independent sites. Putative causal genes were enriched for known mitochondrial DNA depletion syndromes (p = 3.09 × 10−15) and the gene ontology (GO) terms for mtDNA metabolism (p = 1.43 × 10−8) and mtDNA replication (p = 1.2 × 10−7). A clustering approach leveraged pleiotropy between mtDNA-CN associated SNPs and 42 mtDNA-CN associated phenotypes to identify functional domains, revealing five distinct groups, including platelet activation, megakaryocyte proliferation, and mtDNA metabolism. In conclusion, in a GWAS of mtDNA-CN conducted in >450,000 individuals, we identified SNPs within loci that implicate novel pathways that provide a framework for defining the underlying mechanisms involved in genetic control of mtDNA-CN.

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Section: Discussionsupporting

confidence: 87%

Section: Discussionmentioning

confidence: 70%

Section: Discussionmentioning

confidence: 77%

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Genetic analysis of mitochondrial DNA copy number and associated traits identifies loci implicated in nucleotide metabolism, platelet activation, and megakaryocyte proliferation, and reveals a causal association of mitochondrial function with mortality

Longchamps

Yang

Castellani

et al. 2021

Preprint

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“…A recently study found that 23blood-derived mtDNA CN is associated with gene expression across multiple tissues and is predictive for incident neurodegenerative disease, which provides evidence supporting the hypothesis that changes in mtDNA in whole blood may reflect metabolic health across multiple systems. 51 Second, though we accounted for confounders and known batch effects in mtDNA CN and harmonized metabolic traits, we still observed moderate to high heterogeneity in the association coefficients in meta-analysis of most of the phenotypes in both ancestry-specific analyses and across ancestries. Different distributions of age, sex, and phenotypes across study cohorts may partially explain the heterogeneity in these associations.…”

Section: Strengths and Limitationsmentioning

confidence: 82%

Association of mitochondrial DNA copy number with cardiometabolic diseases in a large cross-sectional study of multiple ancestries

Longchamps

Wiggins

et al. 2020

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The mitochondrial genome (mtDNA) is represented at variable copy number (CN) in human cells and plays essential roles in cellular metabolism. Previous studies reported inconsistent associations between mtDNA CN and cardiometabolic disease (CMD) traits. We determined the cross-sectional association of mtDNA CN measured in whole blood with several CMD traits in ∼66,100 individuals (mean age 60, 54% women, and 21% non-European ancestries). Cohort- and ancestry-specific association and meta-analysis were performed adjusting for trait-specific covariates and batch. Because white blood cell (WBC) count, a marker of subclinical inflammation, is associated with mtDNA CN level and multiple CMD traits, we further compared associations with and without adjustment for WBCs in a subset of individuals with WBCs. In meta-analysis without cell count adjustment in European ancestry (EA) participants (n=52,500), lower mtDNA CN was associated with higher odds of obesity (OR with 95% CI=1.13 (1.11, 1.16), P=3.3e-30) and hypertension (OR=1.05 (1.03, 1.08), P=4.0e-07). Further adjusting for WBCs in a subset of EA participants (N=44,100), associations became non-significant (P>0.05) for hypertension, attenuated for obesity (ORwithout cell counts=1.15 (1.12, 1.18) versus ORcell counts=1.06 (1.03, 1.08)) but strengthened for hyperlipidemia (ORwithout cell counts =1.03 (1.00, 1.06) versus ORcell counts =1.06 (1.03, 1.09)). The magnitude and directionality of most associations were consistent between participants of European and other ancestries. Understanding the role of mtDNA CN in CMD will provide insight into the pathobiology underlying metabolic diseases. Further research on modifiable factors that influence mtDNA CN may help develop therapeutic strategies for preventing and treating metabolic diseases.

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“…Similar results were reported for other neurodegenerative diseases (Filograna et al, 2020). Interestingly, although mtDNAcn derived from whole blood is often confounded by variation in cell type composition between individuals, a recent study found an association with AD suggesting that the mtDNAcn in whole blood could potentially reflect metabolic health across tissues (Yang et al, 2021). While the mtDNAcn overall seems to be reduced in brain regions affected by neurodegenerative diseases, mixed results have been reported for the effect of aging on mtDNAcn.…”

Section: Introductionmentioning

confidence: 99%

Characterization of mitochondrial DNA quantity and quality in the human aged and Alzheimer’s disease brain

Klein

Trumpff

Yang

et al. 2021

Preprint

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Mitochondrial dysfunction is a feature of neurodegenerative diseases, including Alzheimer's disease (AD). Using whole-genome sequencing, we assessed mitochondrial DNA (mtDNA) heteroplasmy levels and mtDNA copy number (mtDNAcn) in 1,361 human brain samples of five brain regions from three studies. Multivariable analysis of ten common brain pathologies identified tau pathology in the dorsolateral prefrontal cortex and TDP-43 pathology in the posterior cingulate cortex as primary drivers of reduced mtDNAcn in the aged human brain. Amyloid-β pathology, age, and sex were not associated with mtDNAcn. Further, there is evidence for a direct effect of mitochondrial health on cognition. In contrast, while mtDNA heteroplasmy levels increase by about 1.5% per year of life in the cortical regions, we found little evidence for an association with brain pathologies or cognitive functioning. Thus, our data indicates that mtDNA heteroplasmy burden is unlikely to be involved in the pathogenesis of late-onset neurodegenerative diseases.

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Blood-derived mitochondrial DNA copy number is associated with gene expression across multiple tissues and is predictive for incident neurodegenerative disease

Cited by 15 publications

References 76 publications

Genetic analysis of mitochondrial DNA copy number and associated traits identifies loci implicated in nucleotide metabolism, platelet activation, and megakaryocyte proliferation, and reveals a causal association of mitochondrial function with mortality

Genetic analysis of mitochondrial DNA copy number and associated traits identifies loci implicated in nucleotide metabolism, platelet activation, and megakaryocyte proliferation, and reveals a causal association of mitochondrial function with mortality

Association of mitochondrial DNA copy number with cardiometabolic diseases in a large cross-sectional study of multiple ancestries

Characterization of mitochondrial DNA quantity and quality in the human aged and Alzheimer’s disease brain

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