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Transcriptional Regulation of Important Cellular Processes in Skeletal Myogenesis Through Interferon-γ
16
Citations
51
References
2014
Year
Global Gene ExpressionMolecular RegulationImmunologyCell ProliferationCellular PhysiologyTranscriptional RegulationTissue DevelopmentCell RegulationSkeletal MyogenesisCell SignalingMolecular SignalingHealth SciencesTranscriptomic ProfileSkeletal BiologyGene ExpressionEpigenetic RegulationCell BiologyTranscription RegulationCytokineDevelopmental BiologyGene RegulationTranscription FactorsMedicineImportant Cellular ProcessesCell Development
The purpose of the present study was to investigate the effect of interferon (IFN)-γ on the transcriptomic profile of differentiating mouse C2C12 myogenic cells. Global gene expression was evaluated using whole mouse genome oligonucleotide microarrays, and the results were validated through real-time PCR. IFN-γ (1 ng/mL) increased myoblast proliferation but decreased cell respiration and myosin heavy chain content and slightly decreased the fusion index in differentiating C2C12 cell cultures. The genes upregulated through IFN-γ were involved in cell cycle; regulation of cell proliferation; programmed cell death; chemotaxis; and cytokine, growth factor, and peptidase activity, whereas the genes downregulated through IFN-γ primarily contributed to the regulation of transcription, cell-cell signaling, nitrogen compound biosynthesis, ser/thr protein kinase signaling, and regulation of the Wnt pathway. In conclusion, IFN-γ affects the expression of numerous genes associated with the regulation of several processes in myogenesis. The effects of IFN-γ on cellular transcription include (1) alteration of cytokine/growth factor expression, promoting cell proliferation and migration but inhibiting differentiation, (2) impairment of pro-myogenic transcription, (3) disruption of cell adhesion and sarcolemma/cytoskeleton organization, and (4) increased peptidase activity leading to enhanced proteolysis and apoptosis.
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