4.8 Article

Nuclear numbers in syncytial muscle fibers promote size but limit the development of larger myonuclear domains

Journal

NATURE COMMUNICATIONS
Volume 11, Issue 1, Pages -

Publisher

NATURE RESEARCH
DOI: 10.1038/s41467-020-20058-7

Keywords

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Funding

  1. Cincinnati Children's Hospital Research Foundation
  2. National Institutes of Health [R01 HL130356, R56 HL139680, R01 AR067279, R01 HL105826, R01 HL143490, R13 HL149313, R01AR068286, R01AG059605]
  3. Pew Charitable Trusts
  4. US-Norway Fulbright Foundation for Educational Exchange
  5. Norwegian Research Council [240374]
  6. Medical Research Council of the UK [MR/S023593/1]
  7. American Heart Association [19UFEL34380251, 19TPA34830084]
  8. MyoKardia
  9. AstraZeneca
  10. Merck
  11. Amgen
  12. American Heart Association Postdoctoral Fellowhip [19POST34380448]
  13. MRC [MR/S023593/1] Funding Source: UKRI

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Mammalian cells exhibit remarkable diversity in cell size, but the factors that regulate establishment and maintenance of these sizes remain poorly understood. This is especially true for skeletal muscle, comprised of syncytial myofibers that each accrue hundreds of nuclei during development. Here, we directly explore the assumed causal relationship between multinucleation and establishment of normal size through titration of myonuclear numbers during mouse neonatal development. Three independent mouse models, where myonuclear numbers were reduced by 75, 55, or 25%, led to the discovery that myonuclei possess a reserve capacity to support larger functional cytoplasmic volumes in developing myofibers. Surprisingly, the results revealed an inverse relationship between nuclei numbers and reserve capacity. We propose that as myonuclear numbers increase, the range of transcriptional return on a per nuclear basis in myofibers diminishes, which accounts for both the absolute reliance developing myofibers have on nuclear accrual to establish size, and the limits of adaptability in adult skeletal muscle. Skeletal muscle is composed of syncytial myofibres, each containing hundreds of nuclei. Through genetic reduction of the number of nuclei per myofibre, the authors confirm that more nuclei produce larger cells but myofibres with fewer nuclei adaptively compensate leading to larger and functional myonuclear domains.

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