Somatic mutations in single human cardiomyocytes reveal age-associated DNA damage and widespread oxidative genotoxicity.
Sangita ChoudhuryAugust Yue HuangJunho KimZinan ZhouKatherine MorilloEduardo A MauryJessica W TsaiMichael B MillerMichael A LodatoSarah AratenNazia HilalEunjung Alice LeeMing Hui ChenChristopher A WalshPublished in: Nature aging (2022)
The accumulation of somatic DNA mutations over time is a hallmark of aging in many dividing and nondividing cells but has not been studied in postmitotic human cardiomyocytes. Using single-cell whole-genome sequencing, we identified and characterized the landscape of somatic single-nucleotide variants (sSNVs) in 56 single cardiomyocytes from 12 individuals (aged from 0.4 to 82 years). Cardiomyocyte sSNVs accumulate with age at rates that are faster than in many dividing cell types and nondividing neurons. Cardiomyocyte sSNVs show distinctive mutational signatures that implicate failed nucleotide excision repair and base excision repair of oxidative DNA damage, and defective mismatch repair. Since age-accumulated sSNVs create many damaging mutations that disrupt gene functions, polyploidization in cardiomyocytes may provide a mechanism of genetic compensation to minimize the complete knockout of essential genes during aging. Age-related accumulation of cardiac mutations provides a paradigm to understand the influence of aging on cardiac dysfunction.
Keyphrases
- copy number
- single cell
- dna damage
- genome wide
- high glucose
- endothelial cells
- oxidative stress
- rna seq
- left ventricular
- dna methylation
- induced apoptosis
- dna repair
- high throughput
- induced pluripotent stem cells
- pluripotent stem cells
- angiotensin ii
- spinal cord
- stem cells
- gene expression
- bone marrow
- signaling pathway
- spinal cord injury
- oxide nanoparticles