Sirt2 epigenetically down-regulates PDGFRα expression and promotes CG4 cell differentiation

Fang, Na; Cheng, Junjun; Zhang, Chu; Chen, Keyuan; Zhang, Chenyu; Hu, Zhiping; Bi, Ran; Furber, Kendra L.; Thangaraj, Merlin P.; Nazarali, Adil J.; Ji, Shaoping

doi:10.1080/15384101.2019.1609818

Cited by 9 publications

(9 citation statements)

References 41 publications

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“…Different from functions of the above genes in myogenesis, PDGFRα + mesenchymal progenitors were the major contributor to ectopic fat formation in skeletal muscle [ 37 ], and embryonic adipose progenitor cells without PDGFRα would undergo fate change from adipogenic to fibrotic lineage [ 64 ]. Although DNA methylation-induced PDGFRα and FGFR2 silencing has been reported in CG4 cells [ 65 ] or primary human pituitary adenomas [ 66 ], the role of DNA methylation in regulating the expression level of these co-different genes and their effects on myogenesis or adipogenesis still remains unclear. Unlike the well-known functions of the above genes in ectopic fat accumulation and skeletal muscle development, the function of CNCNA2D2 in relation to skeletal muscle development and homeostasis has been sparsely described in previous studies.…”

Section: Discussionmentioning

confidence: 99%

Global DNA methylation pattern involved in the modulation of differentiation potential of adipogenic and myogenic precursors in skeletal muscle of pigs

Zhang

Sun

et al. 2020

Stem Cell Res Ther

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Background Skeletal muscle is a complex and heterogeneous tissue accounting for approximately 40% of body weight. Excessive ectopic lipid accumulation in the muscle fascicle would undermine the integrity of skeletal muscle in humans but endow muscle with marbling-related characteristics in farm animals. Therefore, the balance of myogenesis and adipogenesis is of great significance for skeletal muscle homeostasis. Significant DNA methylation occurs during myogenesis and adipogenesis; however, DNA methylation pattern of myogenic and adipogenic precursors derived from skeletal muscle remains unknown yet. Methods In this study, reduced representation bisulfite sequencing was performed to analyze genome-wide DNA methylation of adipogenic and myogenic precursors derived from the skeletal muscle of neonatal pigs. Integrated analysis of DNA methylation and transcription profiles was further conducted. Based on the results of pathway enrichment analysis, myogenic precursors were transfected with CACNA2D2-overexpression plasmids to explore the function of CACNA2D2 in myogenic differentiation. Results As a result, 11,361 differentially methylated regions mainly located in intergenic region and introns were identified. Furthermore, 153 genes with different DNA methylation and gene expression level between adipogenic and myogenic precursors were characterized. Subsequently, pathway enrichment analysis revealed that DNA methylation programing was involved in the regulation of adipogenic and myogenic differentiation potential through mediating the crosstalk among pathways including focal adhesion, regulation of actin cytoskeleton, MAPK signaling pathway, and calcium signaling pathway. In particular, we characterized a new role of CACNA2D2 in inhibiting myogenic differentiation by suppressing JNK/MAPK signaling pathway. Conclusions This study depicted a comprehensive landmark of DNA methylome of skeletal muscle-derived myogenic and adipogenic precursors, highlighted the critical role of CACNA2D2 in regulating myogenic differentiation, and illustrated the possible regulatory ways of DNA methylation on cell fate commitment and skeletal muscle homeostasis.

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Section: Discussionmentioning

confidence: 99%

Global DNA methylation pattern involved in the modulation of differentiation potential of adipogenic and myogenic precursors in skeletal muscle of pigs

Zhang

Sun

et al. 2020

Stem Cell Res Ther

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“… 78 Nevertheless, these studies are based on the inhibition of Stat1 pathway in all somatic cells, the influence of Stat1 pathway regulation on remyelination specifically in microglia needs further study. Although the factors such as Pdgfa and Pdgfb secreted by microglia and receptor Pdgfra, Gpr37l1 on OPCs can hinder the differentiation of OPCs, 43 , 48 functional changes revealed by GO analysis in aged OPCs showed no hint of their roles. However, our analysis did not exclude their possible influences and more efforts are needed for further investigation.…”

Section: Discussionmentioning

confidence: 97%

“…37,43 Apoe, App, Pdgfa, Pdgfb and Sdc4 were included in the myelin impediment group (Figure 6B) due to their potential hindrance in OPC differentiation. 48,49 Beneficial cytokines Vegfb and Igf1 did not show significantly high expression in activated microglia (Figure 6B). Subsequently, we attempted to identify several regulatory factors that can upregulate those factors in the myelin promotion group and down-regulate those factors in the myelin impediment group.…”

Section: Regulation Of Stat1 Might Reverse Aged Microglia To Promote Remyelinationmentioning

confidence: 92%

Microglia Impede Oligodendrocyte Generation in Aged Brain

Li¹,

Qi²,

Feng³

et al. 2021

JIR

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Purpose Age-related increase in myelin loss may be responsible for brain atrophy, and the mechanism is not completely understood. We aim to comprehensively delineate oligodendrocyte heterogeneity in young and aged mice and to reveal the underlying mechanism for myelin loss during aging. Methods Diffusion tensor imaging and immunofluorescent staining were performed to verify the demyelination in the aged brains of both rodents and human. Further, the single-cell RNA sequencing data of all brain cells from young and aged mice were deeply analyzed to identify the subsets of oligodendrocyte lineage cells. Cell-to-cell interaction analysis was performed to detect the mechanism of observed changes in oligodendrocyte generation. Results Oligodendrocytes were observed to up-regulate several senescence associated genes in aged brain. Four clusters of oligodendrocyte precursor cells (OPCs) were identified in both young and aged brains. The number of those OPCs in basal state was significantly increased, while the OPCs in the procedure of differentiation were immensely decreased in aged brain. Furthermore, it was identified that activated microglia in the aged brain released inflammatory factors to suppress OPC differentiation. Stat1 might be a potential target to transform senescent microglia into tissue repair type to promote oligodendrocyte generation. Conclusion These results provided a perspective on how age activated microglia could impede remyelination and might give a new therapeutic target for age-related remyelinating diseases.

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“…Cytoplasmic Sirt2 deacetylates multiple proteins, including alpha-tubulin in cultured OPCs 19 and HeLa cells 20 , as well as the polarity protein Par-3 in Schwann cells 21 . Sirt2 also suppressed PDGFRα expression after translocation to the nucleus, promoting differentiation of the CG4 glial cell line 22 . In addition, a recent study found that Sirt2 is delivered to axons from OL to promote mitochondrial ATP production 23 .…”

Section: Introductionmentioning

confidence: 94%

Sirt2 promotes white matter oligodendrogenesis during development and in models of neonatal hypoxia

et al. 2022

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Delayed oligodendrocyte (OL) maturation caused by hypoxia (Hx)-induced neonatal brain injury results in hypomyelination and leads to neurological disabilities. Previously, we characterized Sirt1 as a crucial regulator of OL progenitor cell (OPC) proliferation in response to Hx. We now identify Sirt2 as a critical promoter of OL differentiation during both normal white matter development and in a mouse model of Hx. Importantly, we find that Hx reduces Sirt2 expression in mature OLs and that Sirt2 overexpression in OPCs restores mature OL populations. Reduced numbers of Sirt2+ OLs were also observed in the white matter of preterm human infants. We show that Sirt2 interacts with p27Kip1/FoxO1, p21Cip1/Cdk4, and Cdk5 pathways, and that these interactions are altered by Hx. Furthermore, Hx induces nuclear translocation of Sirt2 in OPCs where it binds several genomic targets. Overall, these results indicate that a balance of Sirt1 and Sirt2 activity is required for developmental oligodendrogenesis, and that these proteins represent potential targets for promoting repair following white matter injury.

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Sirt2 epigenetically down-regulates PDGFRα expression and promotes CG4 cell differentiation

Cited by 9 publications

References 41 publications

Global DNA methylation pattern involved in the modulation of differentiation potential of adipogenic and myogenic precursors in skeletal muscle of pigs

Global DNA methylation pattern involved in the modulation of differentiation potential of adipogenic and myogenic precursors in skeletal muscle of pigs

Microglia Impede Oligodendrocyte Generation in Aged Brain

Sirt2 promotes white matter oligodendrogenesis during development and in models of neonatal hypoxia

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