Mitochondrial haplotype modulates genome expression and mitochondrial structure/function in cardiomyocytes following volume overload.
Jason L GuichardMariame Selma KaneMaximiliano GrenettMichael SandelGloria A BenavidesWayne E BradleyPamela Cox PowellVictor Darley-UsmarScott W BallingerLouis J Dell'ItaliaPublished in: American journal of physiology. Heart and circulatory physiology (2023)
Mitochondrial DNA (mtDNA) haplotype regulates mitochondrial structure/function and reactive oxygen species in aortocaval fistula (ACF) in mice. Here, we unravel the mitochondrial haplotype effects on cardiomyocyte mitochondrial ultrastructure and transcriptome response to ACF in vivo. Phenotypic responses and quantitative transmission electron microscopy (TEM) and RNA sequence at 3 days were determined after sham surgery or ACF in vivo in cardiomyocytes from wild-type (WT) C57BL/6J (C57 n :C57 mt ) and C3H/HeN (C3H n :C3H mt ) and mitochondrial nuclear exchange mice (C57 n :C3H mt or C3H n :C57 mt ). Quantitative TEM of cardiomyocyte mitochondria C3HWT hearts have more electron-dense compact mitochondrial cristae compared with C57WT. In response to ACF, mitochondrial area and cristae integrity are normal in C3HWT; however, there is mitochondrial swelling, cristae lysis, and disorganization in both C57WT and MNX hearts. Tissue analysis shows that C3HWT hearts have increased autophagy, antioxidant, and glucose fatty acid oxidation-related genes compared with C57WT. Comparative transcriptomic analysis of cardiomyocytes from ACF was dependent upon mtDNA haplotype. C57mtDNA haplotype was associated with increased inflammatory/protein synthesis pathways and downregulation of bioenergetic pathways, whereas C3HmtDNA showed upregulation of autophagy genes. In conclusion, ACF in vivo shows a protective response of C3Hmt haplotype that is in large part driven by mitochondrial nuclear genome interaction. NEW & NOTEWORTHY The results of this study support the effects of mtDNA haplotype on nuclear gene expression in cardiomyocytes. Currently, there is no acceptable therapy for volume overload due to mitral regurgitation. The findings of this study could suggest that mtDNA haplotype activates different pathways after ACF warrants further investigations on human population of heart disease from different ancestry backgrounds.
Keyphrases
- oxidative stress
- mitochondrial dna
- copy number
- gene expression
- reactive oxygen species
- signaling pathway
- genome wide
- cell death
- poor prognosis
- fatty acid
- cell proliferation
- wild type
- dna methylation
- nitric oxide
- type diabetes
- minimally invasive
- electron microscopy
- rna seq
- blood pressure
- angiotensin ii
- high resolution
- metabolic syndrome
- pulmonary hypertension
- coronary artery disease
- blood glucose
- weight loss
- low cost