Scientific Reports (Jan 2023)

Continuous exposure to isoprenaline reduced myotube size by delaying myoblast differentiation and fusion through the NFAT-MEF2C signaling pathway

  • Jing Yue,
  • Wei Xu,
  • Li Xiang,
  • Shao-juan Chen,
  • Xin-yuan Li,
  • Qian Yang,
  • Ruo-nan Zhang,
  • Xin Bao,
  • Yan Wang,
  • MagdaleenaNaemi Mbadhi,
  • Yun Liu,
  • Lu-yuan Yao,
  • Long Chen,
  • Xiao-ying Zhao,
  • Chang-qing Hu,
  • Jing-xuan Zhang,
  • Hong-tao Zheng,
  • Yan Wu,
  • Shi-You Chen,
  • Shan Li,
  • Jing Lv,
  • Liu-liu Shi,
  • Jun-ming Tang

DOI
https://doi.org/10.1038/s41598-022-22330-w
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 17

Abstract

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Abstract We aimed to explore whether superfluous sympathetic activity affects myoblast differentiation, fusion, and myofiber types using a continuous single-dose isoprenaline exposure model in vitro and to further confirm the role of distinct NFATs in ISO-mediated effects. Compared with delivery of single and interval single, continuous single-dose ISO most obviously diminished myotube size while postponing myoblast differentiation/fusion in a time- and dose-dependent pattern, accompanied by an apparent decrease in nuclear NFATc1/c2 levels and a slight increase in nuclear NFATc3/c4 levels. Overexpression of NFATc1 or NFATc2, particularly NFATc1, markedly abolished the inhibitory effects of ISO on myoblast differentiation/fusion, myotube size and Myh7 expression, which was attributed to a remarkable increase in the nuclear NFATc1/c2 levels and a reduction in the nuclear NFATc4 levels and the associated increase in the numbers of MyoG and MEF2C positive nuclei within more than 3 nuclei myotubes, especially in MEF2C. Moreover, knockdown of NFATc3 by shRNA did not alter the inhibitory effect of ISO on myoblast differentiation/fusion or myotube size but partially recovered the expression of Myh7, which was related to the slightly increased nuclear levels of NFATc1/c2, MyoG and MEF2C. Knockdown of NFATc4 by shRNA prominently increased the number of MyHC +, MyoG or MEF2C + myoblast cells with 1 ~ 2 nuclei, causing fewer numbers and smaller myotube sizes. However, NFATc4 knockdown further deteriorated the effects of ISO on myoblast fusion and myotube size, with more than 5 nuclei and Myh1/2/4 expression, which was associated with a decrease in nuclear NFATc2/c3 levels. Therefore, ISO inhibited myoblast differentiation/fusion and myotube size through the NFAT-MyoG-MEF2C signaling pathway.