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Ross, Jacob A.; Levy, Yotam; Svensson, Kristoffer; Philp, Andrew; Schenk, Simon; Ochala, Julien
Journal of cellular physiology, September 2018, Letnik: 233, Številka: 9Journal Article
Skeletal muscle fibers are giant multinucleated cells wherein individual nuclei govern the protein synthesis in a finite volume of cytoplasm; this is termed the myonuclear domain (MND). The factors that control MND size remain to be defined. In the present study, we studied the contribution of the NAD+‐dependent deacetylase, sirtuin 1 (SIRT1), to the regulation of nuclear number and MND size. For this, we isolated myofibers from mice with tissue‐specific inactivation (mKO) or inducible overexpression (imOX) of SIRT1 and analyzed the 3D organisation of myonuclei. In imOX mice, the number of nuclei was increased whilst the average MND size was decreased as compared to littermate controls. Our findings were the opposite in mKO mice. Muscle stem cell (satellite cell) numbers were reduced in mKO muscles, a possible explanation for the lower density of myonuclei in these mice; however, no change was observed in imOX mice, suggesting that other factors might also be involved, such as the functional regulation of stem cells/muscle precursors. Interestingly, however, the changes in the MND volume did not impact the force‐generating capacity of muscle fibers. Taken together, our results demonstrate that SIRT1 is a key regulator of MND sizes, although the underlying molecular mechanisms and the cause‐effect relationship between MND and muscle function remain to be fully defined. Overexpression of SIRT1 increases myonuclear density and thus reduces myonuclear domain sizes; conversely, ablation of SIRT1 decreases myonuclear density and thus increases myonuclear domain volumes. Altered satellite cell numbers might explain such modulation of myonuclear density within muscle fibers.
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