Cathepsin S activity controls chronic stress-induced muscle atrophy and dysfunction in mice.
Ying WanLimei PiaoShengnan XuXiangkun MengZhe HuangAiko InoueHailong WangXueling YueXueying JinYongshan NanGuo-Ping ShiToyoaki MuroharaHiroyuki UmegakiMasafumi KuzuyaXian Wu ChengPublished in: Cellular and molecular life sciences : CMLS (2023)
Exposure to chronic psychological stress (CPS) is an intractable risk factor for inflammatory and metabolic diseases. Lysosomal cysteinyl cathepsins play an important role in human pathobiology. Given that cathepsin S (CTSS) is upregulated in the stressed vascular and adipose tissues, we investigated whether CTSS participates in chronic stress-induced skeletal muscle mass loss and dysfunction, with a special focus on muscle protein metabolic imbalance and apoptosis. Eight-week-old male wildtype (CTSS +/+ ) and CTSS-knockout (CTSS -/- ) mice were randomly assigned to non-stress and variable-stress groups. CTSS +/+ stressed mice showed significant losses of muscle mass, dysfunction, and fiber area, plus significant mitochondrial damage. In this setting, stressed muscle in CTSS +/+ mice presented harmful alterations in the levels of insulin receptor substrate 2 protein content (IRS-2), phospho-phosphatidylinositol 3-kinase, phospho-protein kinase B, and phospho-mammalian target of rapamycin, forkhead box-1, muscle RING-finger protein-1 protein, mitochondrial biogenesis-related peroxisome proliferator-activated receptor-γ coactivator-α, and apoptosis-related B-cell lymphoma 2 and cleaved caspase-3; these alterations were prevented by CTSS deletion. Pharmacological CTSS inhibition mimics its genetic deficiency-mediated muscle benefits. In C 2 C 12 cells, CTSS silencing prevented stressed serum- and oxidative stress-induced IRS-2 protein reduction, loss of the myotube myosin heavy chain content, and apoptosis accompanied by a rectification of investigated molecular harmful changes; these changes were accelerated by CTSS overexpression. These findings demonstrated that CTSS plays a role in IRS-2-related protein anabolism and catabolism and cell apoptosis in stress-induced muscle wasting, suggesting a novel therapeutic strategy for the control of chronic stress-related muscle disease in mice under our experimental conditions by regulating CTSS activity.
Keyphrases
- stress induced
- oxidative stress
- protein protein
- skeletal muscle
- cell cycle arrest
- high fat diet induced
- induced apoptosis
- cell death
- protein kinase
- endoplasmic reticulum stress
- binding protein
- type diabetes
- small molecule
- endothelial cells
- insulin resistance
- transcription factor
- cell proliferation
- gene expression
- adipose tissue
- metabolic syndrome
- pi k akt
- depressive symptoms
- clinical trial
- heat stress
- copy number
- high speed
- study protocol
- pluripotent stem cells
- glycemic control