4.7 Article

Displaced Myonuclei in Cancer Cachexia Suggest Altered Innervation

期刊

出版社

MDPI
DOI: 10.3390/ijms21031092

关键词

Central nuclei; muscle regeneration; striated muscles; c26-colon carcinoma; cancer cachexia; altered innervation

资金

  1. Agence Nationale de la Recherche [17-CE17-0015-01, 13-BSV1-0005]
  2. National Institutes of Health [5R01CA180057-02]
  3. IBPS Sorbonne Universite
  4. Association Francaise contre les Myopathies [20603-2017, 16282]
  5. Ministero dell'Istruzione, dell'Universita e della Ricerca [PRIN 2009WBFZYM 001, PRIN 2012N8YJC3]
  6. UIF -Universita Italo-Francese: VINCI 2018
  7. Sapienza Universita di Roma: Avvio alla Ricerca 2019

向作者/读者索取更多资源

An idiopathic myopathy characterized by central nuclei in muscle fibers, a hallmark of muscle regeneration, has been observed in cancer patients. In cancer cachexia skeletal muscle is incapable of regeneration, consequently, this observation remains unaccounted for. In C26-tumor bearing, cachectic mice, we observed muscle fibers with central nuclei in the absence of molecular markers of bona fide regeneration. These clustered, non-peripheral nuclei were present in NCAM-expressing muscle fibers. Since NCAM expression is upregulated in denervated myofibers, we searched for additional makers of denervation, including AchRs, MUSK, and HDAC. This last one being also consistently upregulated in cachectic muscles, correlated with an increase of central myonuclei. This held true in the musculature of patients suffering from gastrointestinal cancer, where a progressive increase in the number of central myonuclei was observed in weight stable and in cachectic patients, compared to healthy subjects. Based on all of the above, the presence of central myonuclei in cancer patients and animal models of cachexia is consistent with motor neuron loss or NMJ perturbation and could underlie a previously neglected phenomenon of denervation, rather than representing myofiber damage and regeneration in cachexia. Similarly to aging, denervation-dependent myofiber atrophy could contribute to muscle wasting in cancer cachexia.

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