4.8 Article

Somatic mutagenesis in satellite cells associates with human skeletal muscle aging

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NATURE COMMUNICATIONS
卷 9, 期 -, 页码 -

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NATURE PUBLISHING GROUP
DOI: 10.1038/s41467-018-03244-6

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资金

  1. Swedish Research Council
  2. Center for Innovative Medicine
  3. Hagelen Foundation
  4. Osterman Foundation
  5. Svenska Lakaresallskapet
  6. Stohnes Foundation
  7. INFERNET [734439]
  8. Swedish Medical Research Council [2013-09305]
  9. Marcus and Marianne Wallenberg foundation
  10. Wallenberg Foundation
  11. Science for Life Laboratory
  12. Knut and Alice Wallenberg Foundation
  13. National Genomics Infrastructure - the Swedish Research Council
  14. Mutation Analysis Core Facility (MAF) at the Karolinska University Hospital
  15. Swedish Research Council [2013-09305] Funding Source: Swedish Research Council

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Human aging is associated with a decline in skeletal muscle (SkM) function and a reduction in the number and activity of satellite cells (SCs), the resident stem cells. To study the connection between SC aging and muscle impairment, we analyze the whole genome of single SC clones of the leg muscle vastus lateralis from healthy individuals of different ages (21-78 years). We find an accumulation rate of 13 somatic mutations per genome per year, consistent with proliferation of SCs in the healthy adult muscle. SkM-expressed genes are protected from mutations, but aging results in an increase in mutations in exons and promoters, targeting genes involved in SC activity and muscle function. In agreement with SC mutations affecting the whole tissue, we detect a missense mutation in a SC propagating to the muscle. Our results suggest somatic mutagenesis in SCs as a driving force in the age-related decline of SkM function.

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