Oxidative stress-induced premature senescence and aggravated denervated skeletal muscular atrophy by regulating progerin–p53 interaction

Progerin elevates atrophic gene expression and helps modify the nuclear membrane to cause severe muscle pathology, which is similar to muscle weakness in the elderly, to alter the development and function of the skeletal muscles. Stress-induced premature senescence (SIPS), a state of cell growth arr...

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Published inSkeletal muscle Vol. 12; no. 1; pp. 1 - 19
Main Authors Xiang, Yaoxian, You, Zongqi, Huang, Xinying, Dai, Junxi, Zhang, Junpeng, Nie, Shuqi, Xu, Lei, Jiang, Junjian, Xu, Jianguang
Format Journal Article
LanguageEnglish
Published London BioMed Central Ltd 29.07.2022
BioMed Central
BMC
Subjects
Aging
Analysis
Animal models
Antibodies
Apoptosis
Atrophy
Atrophy, Muscular
Denervated muscle atrophy
Denervation
DNA damage
Flow cytometry
Gene deletion
Gene expression
Laboratory animals
Mediation
Muscles
Musculoskeletal system
Nitric oxide
Nitric-oxide synthase
Oxidative stress
P53
p53 Protein
Pathogenesis
Progerin
Proteins
Reactive oxygen species
ROS
Senescence
Skeletal muscle
Thermal cycling
Tumor proteins
China
United Kingdom > UK
United States > US
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Summary:Progerin elevates atrophic gene expression and helps modify the nuclear membrane to cause severe muscle pathology, which is similar to muscle weakness in the elderly, to alter the development and function of the skeletal muscles. Stress-induced premature senescence (SIPS), a state of cell growth arrest owing to such stimuli as oxidation, can be caused by progerin. However, evidence for whether SIPS-induced progerin accumulation is connected to denervation-induced muscle atrophy is not sufficient. Flow cytometry and a reactive oxygen species (ROS) as well as inducible nitric oxide synthase (iNOS) inhibitors were used to assess the effect of oxidation on protein (p53), progerin, and nuclear progerin-p53 interaction in the denervated muscles of models of mice suffering from sciatic injury. Loss-of-function approach with the targeted deletion of p53 was used to assess connection among SIPS, denervated muscle atrophy, and fibrogenesis. The augmentation of ROS and iNOS-derived NO in the denervated muscles of models of mice suffering from sciatic injury upregulates p53 and progerin. The abnormal accumulation of progerin in the nuclear membrane as well as the activation of nuclear progerin-p53 interaction triggered premature senescence in the denervated muscle cells of mice. The p53-dependent SIPS in denervated muscles contributes to their atrophy and fibrogenesis. Oxidative stress-triggered premature senescence via nuclear progerin-p53 interaction that promotes denervated skeletal muscular atrophy and fibrogenesis.
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ISSN:2044-5040
2044-5040
DOI:10.1186/s13395-022-00302-y