Aging and neurodegeneration are associated with increased mutations in single human neurons.
Michael A LodatoRachel E RodinCraig L BohrsonMichael E CoulterAlison R BartonMinseok KwonMaxwell A ShermanCarl M VitzthumLovelace J LuquetteChandri N YandavaPengwei YangThomas W ChittendenNicole E HatemSteven C RyuMollie B WoodworthPeter J ParkChristopher A WalshPublished in: Science (New York, N.Y.) (2017)
It has long been hypothesized that aging and neurodegeneration are associated with somatic mutation in neurons; however, methodological hurdles have prevented testing this hypothesis directly. We used single-cell whole-genome sequencing to perform genome-wide somatic single-nucleotide variant (sSNV) identification on DNA from 161 single neurons from the prefrontal cortex and hippocampus of 15 normal individuals (aged 4 months to 82 years), as well as 9 individuals affected by early-onset neurodegeneration due to genetic disorders of DNA repair (Cockayne syndrome and xeroderma pigmentosum). sSNVs increased approximately linearly with age in both areas (with a higher rate in hippocampus) and were more abundant in neurodegenerative disease. The accumulation of somatic mutations with age-which we term genosenium-shows age-related, region-related, and disease-related molecular signatures and may be important in other human age-associated conditions.
Keyphrases
- gene expression
- prefrontal cortex
- genome wide
- dna methylation
- early onset
- dna repair
- copy number
- endothelial cells
- spinal cord
- single cell
- dna damage
- late onset
- induced pluripotent stem cells
- pluripotent stem cells
- single molecule
- rna seq
- circulating tumor
- case report
- spinal cord injury
- blood brain barrier
- preterm birth