Muscle-restricted nuclear receptor interaction protein knockout causes motor neuron degeneration through down-regulation of myogenin at the neuromuscular junction
Autor: | Hsin-Hsiung, Chen, Li-Kai, Tsai, Kuan-Yu, Liao, Tung-Chien, Wu, Yun-Hsin, Huang, Yuan-Chun, Huang, Szu-Wei, Chang, Pei-Yu, Wang, Yeou-Ping, Tsao, Show-Li, Chen |
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Rok vydání: | 2017 |
Předmět: |
Mice
Knockout Motor Neurons Motor neuron NRIP Neuromuscular Junction Gene Expression Nuclear Proteins Original Articles musculoskeletal system Immunohistochemistry Muscular Dystrophies Mice Phenotype nervous system Transduction Genetic Gene Knockdown Techniques Nerve Degeneration Animals Humans Myogenin Original Article Biomarkers Adaptor Proteins Signal Transducing |
Zdroj: | Journal of Cachexia, Sarcopenia and Muscle |
ISSN: | 2190-6009 |
Popis: | Background Nuclear receptor interaction protein (NRIP) is a calcium/calmodulin (CaM) binding protein. Nuclear receptor interaction protein interacts with CaM to activate calcineurin and CaMKII signalling. The conventional NRIP knockout mice (global knockout) showed muscular abnormality with reduction of muscle oxidative functions and motor function defects. Methods To investigate the role of NRIP on neuromuscular system, we generated muscle‐restricted NRIP knockout mice [conditional knockout (cKO)]. The muscle functions (including oxidative muscle markers and muscle strength) and lumbar motor neuron functions [motor neuron number, axon denervation, neuromuscular junction (NMJ)] were tested. The laser‐captured microdissection at NMJ of skeletal muscles and adenovirus gene therapy for rescued effects were performed. Results The cKO mice showed muscular abnormality with reduction of muscle oxidative functions and impaired motor performances as global knockout mice. To our surprise, cKO mice also displayed motor neuron degeneration with abnormal architecture of NMJ. Specifically, the cKO mice revealed reduced motor neuron number with small neuronal size in lumbar spinal cord as well as denervating change, small motor endplates, and decreased myonuclei number at NMJ in skeletal muscles. To explore the mechanisms, we screened various muscle‐derived factors and found that myogenin is a potential candidate that myogenin expression was lower in skeletal muscles of cKO mice than wild‐type mice. Because NRIP and myogenin were colocalized around acetylcholine receptors at NMJ, we extracted RNA from synaptic and extrasynaptic regions of muscles using laser capture microdissection and showed that myogenin expression was especially lower at synaptic region in cKO than wild‐type mice. Notably, overexpression of myogenin using intramuscular adenovirus encoding myogenin treatment rescued abnormal NMJ architecture and preserved motor neuron death in cKO mice. Conclusions In summary, we demonstrated that deprivation of NRIP decreases myogenin expression at NMJ, possibly leading to abnormal NMJ formation, denervation of acetylcholine receptor, and subsequent loss of spinal motor neuron. Overexpression of myogenin in cKO mice can partially rescue abnormal NMJ architecture and motor neuron death. Therefore, muscular NRIP is a novel trophic factor supporting spinal motor neuron via stabilization of NMJ by myogenin expression. |
Databáze: | OpenAIRE |
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