Sex differences in heart mitochondria regulate diastolic dysfunction.
Yang CaoLaurent VergnesYu-Chen WangCalvin PanKarthickeyan Chella KrishnanTimothy M MooreManuel Rosa-GarridoTodd H KimballZhiqiang ZhouSarada CharugundlaChristoph D RauMarcus M SeldinJessica J WangYibin WangThomas M VondriskaKaren ReueAldons J LusisPublished in: Nature communications (2022)
Heart failure with preserved ejection fraction (HFpEF) exhibits a sex bias, being more common in women than men, and we hypothesize that mitochondrial sex differences might underlie this bias. As part of genetic studies of heart failure in mice, we observe that heart mitochondrial DNA levels and function tend to be reduced in females as compared to males. We also observe that expression of genes encoding mitochondrial proteins are higher in males than females in human cohorts. We test our hypothesis in a panel of genetically diverse inbred strains of mice, termed the Hybrid Mouse Diversity Panel (HMDP). Indeed, we find that mitochondrial gene expression is highly correlated with diastolic function, a key trait in HFpEF. Consistent with this, studies of a "two-hit" mouse model of HFpEF confirm that mitochondrial function differs between sexes and is strongly associated with a number of HFpEF traits. By integrating data from human heart failure and the mouse HMDP cohort, we identify the mitochondrial gene Acsl6 as a genetic determinant of diastolic function. We validate its role in HFpEF using adenoviral over-expression in the heart. We conclude that sex differences in mitochondrial function underlie, in part, the sex bias in diastolic function.
Keyphrases
- heart failure
- left ventricular
- genome wide
- copy number
- mitochondrial dna
- oxidative stress
- blood pressure
- gene expression
- endothelial cells
- poor prognosis
- mouse model
- dna methylation
- atrial fibrillation
- ejection fraction
- escherichia coli
- high fat diet induced
- induced pluripotent stem cells
- machine learning
- type diabetes
- cell death
- long non coding rna