期刊论文详细信息
Skeletal Muscle
Pro-myogenic small molecules revealed by a chemical screen on primary muscle stem cells
Feodor D. Price1  Sean M. Buchanan1  Joel Schneider1  Monica Hayhurst1  Mark N. Matyas1  Amy J. Wagers1  Amanda Wagner Gee1  Mohammadsharif Tabebordbar1  Lee L. Rubin1  Alessandra Castiglioni2 
[1] Harvard University Department of Stem Cell and Regenerative Biology, 7 Divinity Ave, 02138, Cambridge, MA, USA;Harvard University Department of Stem Cell and Regenerative Biology, 7 Divinity Ave, 02138, Cambridge, MA, USA;Cancer Immunology Department, Genentech, 1 DNA Way, 94080, South San Francisco, CA, USA;
关键词: Satellite cells;    Screening;    RET;    GDNF;    Lestaurtinib;    CEP-701;   
DOI  :  10.1186/s13395-020-00248-z
来源: Springer
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【 摘 要 】

Satellite cells are the canonical muscle stem cells that regenerate damaged skeletal muscle. Loss of function of these cells has been linked to reduced muscle repair capacity and compromised muscle health in acute muscle injury and congenital neuromuscular diseases. To identify new pathways that can prevent loss of skeletal muscle function or enhance regenerative potential, we established an imaging-based screen capable of identifying small molecules that promote the expansion of freshly isolated satellite cells. We found several classes of receptor tyrosine kinase (RTK) inhibitors that increased freshly isolated satellite cell numbers in vitro. Further exploration of one of these compounds, the RTK inhibitor CEP-701 (also known as lestaurtinib), revealed potent activity on mouse satellite cells both in vitro and in vivo. This expansion potential was not seen upon exposure of proliferating committed myoblasts or non-myogenic fibroblasts to CEP-701. When delivered subcutaneously to acutely injured animals, CEP-701 increased both the total number of satellite cells and the rate of muscle repair, as revealed by an increased cross-sectional area of regenerating fibers. Moreover, freshly isolated satellite cells expanded ex vivo in the presence of CEP-701 displayed enhanced muscle engraftment potential upon in vivo transplantation. We provide compelling evidence that certain RTKs, and in particular RET, regulate satellite cell expansion during muscle regeneration. This study demonstrates the power of small molecule screens of even rare adult stem cell populations for identifying stem cell-targeting compounds with therapeutic potential.

【 授权许可】

CC BY   

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