4.7 Article

In vivo myomaker-mediated heterologous fusion and nuclear reprogramming

期刊

FASEB JOURNAL
卷 31, 期 1, 页码 400-+

出版社

FEDERATION AMER SOC EXP BIOL
DOI: 10.1096/fj.201600945R

关键词

cell therapy; membrane fusion; muscular dystrophy

资金

  1. Cincinnati Children's Hospital Research Foundation
  2. U.S. National Institutes of Health
  3. National Institute of Arthritis and Musculoskeletal and Skin Diseases [R01AR068286]
  4. Muscular Dystrophy Association
  5. Pew Charitable Trusts

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Knowledge regarding cellular fusion and nuclear reprogramming may aid in cell therapy strategies for skeletal muscle diseases. An issue with cell therapy approaches to restore dystrophin expression in muscular dystrophy is obtaining a sufficient quantity of cells that normally fuse with muscle. Here we conferred fusogenic activity without transdifferentiation to multiple non-muscle cell types and tested dystrophin restoration inmouse models of muscular dystrophy. We previously demonstrated that myomaker, a skeletal muscle-specific transmembrane protein necessary for myoblast fusion, is sufficient to fuse 10T 1/2 fibroblasts to myoblasts in vitro. Whether myomaker-mediated heterologous fusion is functional in vivo and whether the newly introduced nonmuscle nuclei undergoes nuclear reprogramming has not been investigated. We showed that mesenchymal stromal cells, cortical bone stem cells, and tail-tip fibroblasts fuse to skeletal muscle when they express myomaker. These cells restored dystrophin expression in a fraction of dystrophin-deficient myotubes after fusion in vitro. However, dystrophin restoration was not detected in vivo although nuclear reprogramming of the muscle-specific myosin light chain promoter did occur. Despite the lack of detectable dystrophin reprogramming by immunostaining, this study indicated that myomaker could be used in nonmuscle cells to induce fusion with muscle in vivo, thereby providing a platform to deliver therapeutic material.-Mitani, Y., Vagnozzi, R. J., Millay, D. P. In vivo myomaker-mediated heterologous fusion and nuclear reprogramming.

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