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YB-1 gene expression is kept constant during myocyte differentiation through replacement of different transcription factors and then falls gradually under the control of neural activity
Affiliation:1. Department of Electronics and Communications Engineering, Al-Nahrain University, Baghdad, Iraq;2. Department of Electrical Engineering and Electronics, The University of Liverpool, Liverpool L69 3GJ, UK;1. Key Lab for IOT and Information Fusion Technology of Zhejiang, Institute of Information Science and Control, Hangzhou Dianzi University, Hangzhou 310018, PR China;2. Research Institute of Liaoyang Petrochemical Company, PetroChina, PR China;3. China Petroleum Longhui Automation Engineering Co. Ltd., PR China;1. Centro de Investigación y de Estudios Avanzados del Instituto Politécnico Nacional, Guadalajara, Mexico;2. Faculty of Electrical Engineering, Czech Technical University in Prague, Czech Republic;3. Czech Institute of Informatics, Robotics, and Cybernetics, Czech Technical University in Prague, Czech Republic
Abstract:We have previously reported that translation of acetylcholine receptor α-subunit (AChR α) mRNA in skeletal muscle cells is regulated by Y-box binding protein 1 (YB-1) in response to neural activity, and that in the postnatal mouse developmental changes in the amount of YB-1 mRNA are similar to those of AChR α mRNA, which is known to be regulated by myogenic transcription factors. Here, we examined transcriptional regulation of the YB-1 gene in mouse skeletal muscle and differentiating C2C12 myocytes. Although neither YB-1 nor AChR α was detected at either the mRNA or protein level in adult hind limb muscle, YB-1 expression was transiently activated in response to denervation of the sciatic nerve and completely paralleled that of AChR α, suggesting that these genes are regulated by the same transcription factors. However, during differentiation of C2C12 cells to myotubes, the level of YB-1 remained constant even though the level of AChR α increased markedly. Reporter gene, gel mobility shift and ChIP assays revealed that in the initial stage of myocyte differentiation, transcription of the YB-1 gene was regulated by E2F1 and Sp1, and was then gradually replaced under the control of both MyoD and myogenin through an E-box sequence in the proximal region of the YB-1 gene promoter. These results suggest that transcription factors for the YB-1 gene are exchanged during skeletal muscle cell differentiation, perhaps playing a role in translational control of mRNAs by YB-1 in both myotube formation and the response of skeletal muscle tissues to neural stimulation.
Keywords:Skeletal muscle cells  Differentiation  YB-1 gene  Transcription factors
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