FTO is required for myogenesis by positively regulating mTOR-PGC-1α pathway-mediated mitochondria biogenesis

Wang, Xiaobo; Huang, Ning; Yang, Min; Wei, Dandan; Tai, Haoran; Han, Xiaobin; Gong, Hui; Zhou, Jiao; Qin, Jianqiong; Wei, Xiawei; Chen, Honghan; Fang, Tingting; Xiao, Hengyi

doi:10.1038/cddis.2017.122

Cited by 115 publications

(119 citation statements)

References 43 publications

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“…), and skeletal muscle myoblast differentiation (Wang et al . ), all of which suggest the general importance of FTO in development. Consistent with this notion, loss of FTO function in mice and human leads to postnatal growth retardation, including smaller brain volume (Boissel et al .…”

Section: The M6a‐machineriesmentioning

confidence: 89%

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The m6A‐epitranscriptomic signature in neurobiology: from neurodevelopment to brain plasticity

Widagdo

Anggono

2018

Journal of Neurochemistry

120

103

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Research over the past decade has provided strong support for the importance of various epigenetic mechanisms, including DNA and histone modifications in regulating activity-dependent gene expression in the mammalian central nervous system. More recently, the emerging field of epitranscriptomics revealed an equally important role of post-transcriptional RNA modifications in shaping the transcriptomic landscape of the brain. This review will focus on the methylation of the adenosine base at the N6 position, termed N methyladenosine (m6A), which is the most abundant internal modification that decorates eukaryotic messenger RNAs. Given its prevalence and dynamic regulation in the adult brain, the m6A-epitranscriptome provides an additional layer of regulation on RNA that can be controlled in a context- and stimulus-dependent manner. Conceptually, m6A serves as a molecular switch that regulates various aspects of RNA function, including splicing, stability, localization, or translational control. The versatility of m6A function is typically determined through interaction or disengagement with specific classes of m6A-interacting proteins. Here we review recent advances in the field and provide insights into the roles of m6A in regulating brain function, from development to synaptic plasticity, learning, and memory. We also discuss how aberrant m6A signaling may contribute to neurodevelopmental and neuropsychiatric disorders.

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Section: The M6a‐machineriesmentioning

confidence: 89%

“…; Wang et al . ). Given that FTO undergoes nucleocytoplasmic shuttling in cells, it is conceivable that FTO may play a key role in modulating the mTORC1 signaling pathway in the cytoplasm (Russell and Morgan ; Gulati et al .…”

Section: The M6a‐machineriesmentioning

confidence: 97%

The m6A‐epitranscriptomic signature in neurobiology: from neurodevelopment to brain plasticity

Widagdo

Anggono

2018

Journal of Neurochemistry

120

103

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“…41 Recent studies have demonstrated that meclofenamic acid, a highly selective inhibitor of FTO, reduce ROS accumulation and apoptosis, 42 and that FTO regulates mitochondrial function. 35,36 We have been suggested that (Figure 4A,B).…”

Section: Fto Regulates Mitochondrial Biogenesis and Oxidative Phospmentioning

confidence: 98%

“…However, the impact of FTO, especially as an RNA demethylase, in mitochondrial biogenesis, oxidative stress and ccRCC progression remain elusive. Importantly, recent reports suggest that FTO regulate mitochondria content through mediating mitochondrial fusion, fission and biogenesis‐associated genes expression as a N6‐methyladenosine RNA demethylase . To the point, we aim to explore the biological function of FTO in the post‐transcriptional modification of mitochondrial biogenesis and its subsequent influence in ccRCC and also explore the underlying molecular mechanism through identifying its key mRNA targets.…”

Section: Introductionmentioning

confidence: 99%

N6‐methyladenosine demethylase FTO suppresses clear cell renal cell carcinoma through a novel FTO‐PGC‐1α signalling axis

Zhuang

Luo

et al. 2019

J Cellular Molecular Medi

118

106

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The abundant and reversible N6‐methyladenosine (m6A) R NA modification and its modulators have important roles in regulating various gene expression and biological processes. Here, we demonstrate that fat mass and obesity associated ( FTO ), as an m6A demethylase, plays a critical anti‐tumorigenic role in clear cell renal cell carcinoma (cc RCC ). FTO is suppressed in cc RCC tissue. The low expression of FTO in human cc RCC correlates with increased tumour severity and poor patient survival. The Von Hippel‐Lindau‐deficient cells expressing FTO restores mitochondrial activity, induces oxidative stress and ROS production and shows impaired tumour growth, through increasing expression of PGC ‐1α by reducing m6A levels in its mRNA transcripts. Our work demonstrates the functional importance of the m6A methylation and its modulator, and uncovers a critical FTO ‐ PGC ‐1α axis for developing effective therapeutic strategies in the treatment of cc RCC .

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“…Alternatively, mTOR may have a role in OMM signaling through interplay with AKAP‐1, wherein mitochondrial PKA signaling may influence mTOR activity . It is clear that mTOR signaling is highly integrated with mitochondria physiology …”

Section: Other Kinases Associated With Ommmentioning

confidence: 99%

Phosphoregulation on mitochondria: Integration of cell and organelle responses

2019

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Mitochondria are highly integrated organelles that are crucial to cell adaptation and mitigating adverse physiology. Recent studies demonstrate that fundamental signal transduction pathways incorporate mitochondrial substrates into their biological programs. Reversible phosphorylation is emerging as a useful mechanism to modulate mitochondrial function in accordance with cellular changes. Critical serine/threonine protein kinases, such as the c‐Jun N‐terminal kinase (JNK), protein kinase A (PKA), PTEN‐induced kinase‐1 (PINK1), and AMP‐dependent protein kinase (AMPK), readily translocate to the outer mitochondrial membrane (OMM), the interface of mitochondria‐cell communication. OMM protein kinases phosphorylate diverse mitochondrial substrates that have discrete effects on organelle dynamics, protein import, respiratory complex activity, antioxidant capacity, and apoptosis. OMM phosphorylation events can be tempered through the actions of local protein phosphatases, such as mitogen‐activated protein kinase phosphatase‐1 (MKP‐1) and protein phosphatase 2A (PP2A), to regulate the extent and duration of signaling. The central mediators of OMM signal transduction are the scaffold proteins because the relative abundance of these accessory proteins determines the magnitude and duration of a signaling event on the mitochondrial surface, which dictates the biological outcome of a local signal transduction pathway. The concentrations of scaffold proteins, such as A‐kinase anchoring proteins (AKAPs) and Sab (or SH3 binding protein 5—SH3BP5), have been shown to influence neuronal survival and vulnerability, respectively, in models of Parkinson's disease (PD), highlighting the importance of OMM signaling to health and disease. Despite recent progress, much remains to be discovered concerning the mechanisms of OMM signaling. Nonetheless, enhancing beneficial OMM signaling events and inhibiting detrimental protein‐protein interactions on the mitochondrial surface may represent highly selective approaches to restore mitochondrial health and homeostasis and mitigate organelle dysfunction in conditions such as PD.

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FTO is required for myogenesis by positively regulating mTOR-PGC-1α pathway-mediated mitochondria biogenesis

Cited by 115 publications

References 43 publications

The m6A‐epitranscriptomic signature in neurobiology: from neurodevelopment to brain plasticity

The m6A‐epitranscriptomic signature in neurobiology: from neurodevelopment to brain plasticity

N6‐methyladenosine demethylase FTO suppresses clear cell renal cell carcinoma through a novel FTO‐PGC‐1α signalling axis

Phosphoregulation on mitochondria: Integration of cell and organelle responses

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