International Journal of Molecular Sciences (Jun 2023)

Skeletal Muscle-Specific <i>Bis</i> Depletion Leads to Muscle Dysfunction and Early Death Accompanied by Impairment in Protein Quality Control

  • Soon-Young Jung,
  • Tae-Ryong Riew,
  • Hye Hyeon Yun,
  • Ji Hee Lim,
  • Ji-Won Hwang,
  • Sung Won Jung,
  • Hong Lim Kim,
  • Jae-Seon Lee,
  • Mun-Yong Lee,
  • Jeong-Hwa Lee

DOI
https://doi.org/10.3390/ijms24119635
Journal volume & issue
Vol. 24, no. 11
p. 9635

Abstract

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Bcl-2-interacting cell death suppressor (BIS), also called BAG3, plays a role in physiological functions such as anti-apoptosis, cell proliferation, autophagy, and senescence. Whole-body Bis-knockout (KO) mice exhibit early lethality accompanied by abnormalities in cardiac and skeletal muscles, suggesting the critical role of BIS in these muscles. In this study, we generated skeletal muscle-specific Bis-knockout (Bis-SMKO) mice for the first time. Bis-SMKO mice exhibit growth retardation, kyphosis, a lack of peripheral fat, and respiratory failure, ultimately leading to early death. Regenerating fibers and increased intensity in cleaved PARP1 immunostaining were observed in the diaphragm of Bis-SMKO mice, indicating considerable muscle degeneration. Through electron microscopy analysis, we observed myofibrillar disruption, degenerated mitochondria, and autophagic vacuoles in the Bis-SMKO diaphragm. Specifically, autophagy was impaired, and heat shock proteins (HSPs), such as HSPB5 and HSP70, and z-disk proteins, including filamin C and desmin, accumulated in Bis-SMKO skeletal muscles. We also found metabolic impairments, including decreased ATP levels and lactate dehydrogenase (LDH) and creatine kinase (CK) activities in the diaphragm of Bis-SMKO mice. Our findings highlight that BIS is critical for protein homeostasis and energy metabolism in skeletal muscles, suggesting that Bis-SMKO mice could be used as a therapeutic strategy for myopathies and to elucidate the molecular function of BIS in skeletal muscle physiology.

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