A novel potent tumour promoter aberrantly overexpressed in most human cancers

Takahashi, Atsushi; Tokita, Hisashi; Takahashi, Keiichi; Takeoka, Tomoharu; Murayama, Kazuro; Tomotsune, Daihachiro; Ohira, Miki; Iwamatsu, Akihiro; Ohara, Kazuaki; Yazaki, Kazufumi; Koda, Tadayuki; Nakagawara, Akira; Tani, Kenzaburo

doi:10.1038/srep00015

Cited by 21 publications

(47 citation statements)

References 58 publications

(84 reference statements)

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“…The most significant TCG is METTL13 (methyltransferase like 13), which was correlated with sum of NFT density estimates in the superior parietal lobule (BM7-SPL) ( r = 0.70, P value = 1.25 × 10 –8 ). The protein product encoded by this gene is the antiapoptotic protein FEAT, which is also aberrantly overexpressed in various human cancer tissues [37]. Among the list of the top trait correlated genes is AKT2 , which encodes a serine/threonine-protein kinase Akt.…”

Section: Resultsmentioning

confidence: 99%

Integrative network analysis of nineteen brain regions identifies molecular signatures and networks underlying selective regional vulnerability to Alzheimer’s disease

Wang¹,

Roussos²,

McKenzie³

et al. 2016

Genome Med

228

244

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BackgroundAlzheimer’s disease (AD) is the most common form of dementia, characterized by progressive cognitive impairment and neurodegeneration. However, despite extensive clinical and genomic studies, the molecular basis of AD development and progression remains elusive.MethodsTo elucidate molecular systems associated with AD, we developed a large scale gene expression dataset from 1053 postmortem brain samples across 19 cortical regions of 125 individuals with a severity spectrum of dementia and neuropathology of AD. We excluded brain specimens that evidenced neuropathology other than that characteristic of AD. For the first time, we performed a pan-cortical brain region genomic analysis, characterizing the gene expression changes associated with a measure of dementia severity and multiple measures of the severity of neuropathological lesions associated with AD (neuritic plaques and neurofibrillary tangles) and constructing region-specific co-expression networks. We rank-ordered 44,692 gene probesets, 1558 co-expressed gene modules and 19 brain regions based upon their association with the disease traits.ResultsThe neurobiological pathways identified through these analyses included actin cytoskeleton, axon guidance, and nervous system development. Using public human brain single-cell RNA-sequencing data, we computed brain cell type-specific marker genes for human and determined that many of the abnormally expressed gene signatures and network modules were specific to oligodendrocytes, astrocytes, and neurons. Analysis based on disease severity suggested that: many of the gene expression changes, including those of oligodendrocytes, occurred early in the progression of disease, making them potential translational/treatment development targets and unlikely to be mere bystander result of degeneration; several modules were closely linked to cognitive compromise with lesser association with traditional measures of neuropathology. The brain regional analyses identified temporal lobe gyri as sites associated with the greatest and earliest gene expression abnormalities.ConclusionsThis transcriptomic network analysis of 19 brain regions provides a comprehensive assessment of the critical molecular pathways associated with AD pathology and offers new insights into molecular mechanisms underlying selective regional vulnerability to AD at different stages of the progression of cognitive compromise and development of the canonical neuropathological lesions of AD.Electronic supplementary materialThe online version of this article (doi:10.1186/s13073-016-0355-3) contains supplementary material, which is available to authorized users.

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Section: Resultsmentioning

confidence: 99%

Integrative network analysis of nineteen brain regions identifies molecular signatures and networks underlying selective regional vulnerability to Alzheimer’s disease

Wang¹,

Roussos²,

McKenzie³

et al. 2016

Genome Med

228

244

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“…In transgenic mice, Mettl13 ectopic overexpression can drive tumorigenesis in vivo (55). Moreover, gene expression profiling of NIH3T3 cells overexpressing METTL13 dysregulated the RTK and hedgehogsignaling pathways (55). Intriguingly, METTL13 is predicted to have methyltransferase activity, spermidine/spermine synthase activity, or ubiquinone synthase activity, but these functions of METLL13 have not been experimentally demonstrated (55).…”

Section: Discussionmentioning

confidence: 99%

“…However, it has low expression in normal tissues including the testis, brain, and liver (55). In transgenic mice, Mettl13 ectopic overexpression can drive tumorigenesis in vivo (55). Moreover, gene expression profiling of NIH3T3 cells overexpressing METTL13 dysregulated the RTK and hedgehogsignaling pathways (55).…”

Section: Discussionmentioning

confidence: 99%

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Modifier variant of METTL13 suppresses human GAB1–associated profound deafness

Yousaf¹,

Ahmed²,

Giese³

et al. 2018

Journal of Clinical Investigation

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“…Cancers develop from the dysregulation of genes involved in normal development and tissue homeostasis (Garraway & Lander, ; Hanahan & Weinberg, ; Vogelstein et al, ). We have previously found that f aint e xpression in normal tissues, a berrant overexpression in t umors (FEAT), the protein encoded by methyltransferase‐like 13 ( METTL13 ), potently drives tumorigenesis in transgenic mice (Takahashi et al, ). FEAT is aberrantly upregulated in most human cancers including colorectal, pancreatic, prostate, breast, ovary, thyroid, and non‐small‐cell lung cancers.…”

Section: Introductionmentioning

confidence: 99%

FEAT enhances INSL3 expression in testicular Leydig cells

Kobayashi

Murayama

et al. 2018

Genes to Cells

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FEAT, the protein encoded by methyltransferase-like 13 (METTL13), is aberrantly upregulated in most human cancers and potently drives tumorigenesis in vivo; however, its role in normal tissues remains elusive. Immunoblotting has displayed weak FEAT expression in normal human tissues, including the testis. Here, we found that FEAT is expressed in fetal and adult Leydig cells in the testis. FEAT knockdown using siRNA increased primary cilia formation in MA-10 Leydig tumor cells, accompanied by enhanced 5' adenosine monophosphate-activated protein kinase (AMPK) activation. Immunofluorescence analyses of FEAT-silenced MA-10 cells showed diminished insulin-like factor 3 (INSL3) expression. A male Mettl13 mouse developed bilateral intraabdominal cryptorchidism, suggesting defective INSL3 production by fetal Leydig cells. Leydig cells from the mouse showed markedly decreased INSL3 protein by immunohistochemistry. Together, these results suggest that FEAT facilitates the INSL3 production in testicular Leydig cells that is essential for transabdominal testis migration.

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A novel potent tumour promoter aberrantly overexpressed in most human cancers

Cited by 21 publications

References 58 publications

Integrative network analysis of nineteen brain regions identifies molecular signatures and networks underlying selective regional vulnerability to Alzheimer’s disease

Integrative network analysis of nineteen brain regions identifies molecular signatures and networks underlying selective regional vulnerability to Alzheimer’s disease

Modifier variant of METTL13 suppresses human GAB1–associated profound deafness

FEAT enhances INSL3 expression in testicular Leydig cells

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