Sachiko Yamashita Takeuchi, Chirada Dusadeemeelap, Tatsuo Kawamoto, Takuma Matsubara, Shoichiro Kokabu, William N Addison
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引用次数: 0
摘要
微量营养素维生素 C 是维持骨骼肌健康和平衡所必需的。长期以来,维生素 C 的促肌生成作用一直归因于其作为一般抗氧化剂的作用,以及在胶原基质合成和肉碱生物合成中的作用。在这里,我们发现维生素 C 还能作为一种表观遗传化合物发挥作用,通过其作为组蛋白 H3 和 DNA 去甲基化的酶辅助因子的活性,在肌肉生成过程中促进染色质景观的转换。我们利用 C2C12 肌母细胞研究维生素 C 对肌生成的表观遗传效应,观察到用维生素 C 处理细胞会降低全局 H3K9 甲基化,增加 5-hmC 水平。此外,在分化过程中,维生素 C 处理可增强成肌细胞标记基因的表达和肌管的形成。我们发现 KDM7A 是一种组蛋白赖氨酸去甲基化酶,在肌形成过程中明显上调。染色质免疫共沉淀分析表明,KDM7A占据了肌生成转录因子MyoD1的启动子区域,它在该区域促进组蛋白去甲基化。我们还证实,甲基胞嘧啶二氧酶 TET1 和 TET2 是成肌分化所必需的,它们的缺失会削弱维生素 C 对成肌的刺激作用。
The micronutrient vitamin C is essential for the maintenance of skeletal muscle health and homeostasis. The pro-myogenic effects of vitamin C have long been attributed to its role as a general antioxidant agent, as well as its role in collagen matrix synthesis and carnitine biosynthesis. Here, we show that vitamin C also functions as an epigenetic compound, facilitating chromatin landscape transitions during myogenesis through its activity as an enzymatic cofactor for histone H3 and DNA demethylation. Utilizing C2C12 myoblast cells to investigate the epigenetic effects of vitamin C on myogenesis, we observe that treatment of cells with vitamin C decreases global H3K9 methylation and increases 5-hmC levels. Furthermore, vitamin C treatment enhances myoblast marker gene expression and myotube formation during differentiation. We identify KDM7A as a histone lysine demethylase markedly upregulated during myogenesis. Accordingly, knockdown of Kdm7a prevents the pro-myogenic effects of vitamin C. Chromatin immunoprecipitation analysis showed that KDM7A occupies the promoter region of the myogenic transcription factor MyoD1 where it facilitates histone demethylation. We also confirm that the methylcytosine dioxygenases TET1 and TET2 are required for myogenic differentiation and that their loss blunts stimulation of myogenesis by vitamin C. In conclusion, our data suggest that an epigenetic mode of action plays a major role in the myogenic effects of vitamin C.
期刊介绍:
The Journal of Cellular Physiology publishes reports of high biological significance in areas of eukaryotic cell biology and physiology, focusing on those articles that adopt a molecular mechanistic approach to investigate cell structure and function. There is appreciation for the application of cellular, biochemical, molecular and in vivo genetic approaches, as well as the power of genomics, proteomics, bioinformatics and systems biology. In particular, the Journal encourages submission of high-interest papers investigating the genetic and epigenetic regulation of proliferation and phenotype as well as cell fate and lineage commitment by growth factors, cytokines and their cognate receptors and signal transduction pathways that influence the expression, integration and activities of these physiological mediators. Similarly, the Journal encourages submission of manuscripts exploring the regulation of growth and differentiation by cell adhesion molecules in addition to the interplay between these processes and those induced by growth factors and cytokines. Studies on the genes and processes that regulate cell cycle progression and phase transition in eukaryotic cells, and the mechanisms that determine whether cells enter quiescence, proliferate or undergo apoptosis are also welcomed. Submission of papers that address contributions of the extracellular matrix to cellular phenotypes and physiological control as well as regulatory mechanisms governing fertilization, embryogenesis, gametogenesis, cell fate, lineage commitment, differentiation, development and dynamic parameters of cell motility are encouraged. Finally, the investigation of stem cells and changes that differentiate cancer cells from normal cells including studies on the properties and functions of oncogenes and tumor suppressor genes will remain as one of the major interests of the Journal.