Human long non-coding RNAs promote pluripotency and neuronal differentiation by association with chromatin modifiers and transcription factors

Ng, Shi‐Yan; Johnson, Rory; Stanton, Lawrence W.

doi:10.1038/emboj.2011.459

Cited by 475 publications

(500 citation statements)

References 45 publications

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“…However, little is known about their functional involvement in human neural differentiation [37,42]. We also examined the expression patterns of SOX2OT and its two novel variants during the course of neural differentiation of NT2 cells.…”

Section: Discussionmentioning

confidence: 99%

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Two Novel Splice Variants of SOX2OT, SOX2OT-S1, and SOX2OT-S2 are Coupregulated with SOX2 and OCT4 in Esophageal Squamous Cell Carcinoma

et al. 2014

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Long noncoding RNAs (lncRNAs) have emerged as new regulators of stem cell pluripotency and tumorigenesis. The SOX2 gene, a master regulator of pluripotency, is embedded within the third intron of a lncRNA known as SOX2 overlapping transcript (SOX2OT). SOX2OT has been suspected to participate in regulation of SOX2 expression and/or other related processes; nevertheless, its potential involvement in tumor initiation and/or progression is unclear. Here, we have evaluated a possible correlation between expression patterns of SOX2OT and those of master regulators of pluripotency, SOX2 and OCT4, in esophageal squamous cell carcinoma (ESCC) tissue samples. We have also examined its potential function in the human embryonic carcinoma stem cell line, NTERA2 (NT2), which highly expresses SOX2OT, SOX2, and OCT4. Our data revealed a significant coupregulation of SOX2OT along with SOX2 and OCT4 in tumor samples, compared to the non-tumor tissues obtained from the margin of same tumors. We also identified two novel splice variants of SOX2OT (SOX2OT-S1 and SOX2OT-S2) which coupregulated with SOX2 and OCT4 in ESCCs. Suppressing SOX2OT variants caused a profound alteration in cell cycle distribution, including a 5.9 and 6.9 time increase in sub-G1 phase of cell cycle for SOX2OT-S1 and SOX2OT-S2, respectively. The expression of all variants was significantly diminished, upon the induction of neural differentiation in NT2 cells, suggesting their potential functional links to the undifferentiated state of the cells. Our data suggest a part for SOX2OT spliced variants in tumor initiation and/or progression as well as regulating pluripotent state of stem cells. STEM CELLS 2014;32:126-134

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Section: Discussionmentioning

confidence: 99%

“…Accordingly, expression patterns of several lncRNAs correlate with those of pluripotency regulators such as OCT4, Nanog, and SOX2 [37,38]. SOX2 is an intronless gene that lies within the third intron of another gene known as SOX2OT [28].…”

Section: Discussionmentioning

confidence: 99%

Two Novel Splice Variants of SOX2OT, SOX2OT-S1, and SOX2OT-S2 are Coupregulated with SOX2 and OCT4 in Esophageal Squamous Cell Carcinoma

et al. 2014

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“…29 We found that this transcript was almost undetectable both in undifferentiated and in RA-treated BE(2)-C cells (Fig. 2SC).…”

Section: Resultsmentioning

confidence: 78%

Identification of linc-NeD125, a novel long non coding RNA that hosts miR-125b-1 and negatively controls proliferation of human neuroblastoma cells

et al. 2015

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“…Ng et al [41] screened the expression of lncRNAs before and after induction of human ESC differentiation into dopaminergic neurons and found that lncRNA_N1, _N2 and _N3 were weakly but significantly expressed after induction of neuronal differentiation. lncRNA_N1 and lncRNA_N3 might function as scaffolds for the interaction with transcription repressors, repressor element 1 (RE1; also called NRSE) silencing TF (REST; also called NRSF) and a PRC2 protein, suppressor of zeste 12 homologue (SUZ12), respectively, resulting in inhibition of their suppressor activity [41].…”

Section: (A) Long Non-coding Rnasmentioning

confidence: 99%

“…lncRNA_N1 and lncRNA_N3 might function as scaffolds for the interaction with transcription repressors, repressor element 1 (RE1; also called NRSE) silencing TF (REST; also called NRSF) and a PRC2 protein, suppressor of zeste 12 homologue (SUZ12), respectively, resulting in inhibition of their suppressor activity [41]. On the other hand, small modulatory dsRNAs encoding the RE1 sequence were found in the nucleus, where they interacted with the REST complex to promote transcription of RE1-associated genes [42].…”

Section: (A) Long Non-coding Rnasmentioning

confidence: 99%

Epigenetic setting and reprogramming for neural cell fate determination and differentiation

Imamura

Uesaka

Nakashima

2014

Phil. Trans. R. Soc. B

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In the mammalian brain, epigenetic mechanisms are clearly involved in the regulation of self-renewal of neural stem cells and the derivation of their descendants, i.e. neurons, astrocytes and oligodendrocytes, according to the developmental timing and the microenvironment, the 'niche'. Interestingly, local epigenetic changes occur, concomitantly with genome-wide level changes, at a set of gene promoter regions for either down-or upregulation of the gene. In addition, intergenic regions also sensitize the availability of epigenetic modifiers, which affects gene expression through a relatively long-range chromatinic interaction with the transcription regulatory machineries including non-coding RNA (ncRNA) such as promoter-associated ncRNA and enhancer ncRNA. We show that such an epigenetic landscape in a neural cell is statically but flexibly formed together with a variable combination of generally and locally acting nuclear molecules including master transcription factors and cell-cycle regulators. We also discuss the possibility that revealing the epigenetic regulation by the local DNA -RNA -protein assemblies would promote methodological innovations, e.g. neural cell reprogramming, engineering and transplantation, to manipulate neuronal and glial cell fates for the purpose of medical use of these cells.

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Human long non-coding RNAs promote pluripotency and neuronal differentiation by association with chromatin modifiers and transcription factors

Cited by 475 publications

References 45 publications

Two Novel Splice Variants of SOX2OT, SOX2OT-S1, and SOX2OT-S2 are Coupregulated with SOX2 and OCT4 in Esophageal Squamous Cell Carcinoma

Two Novel Splice Variants of SOX2OT, SOX2OT-S1, and SOX2OT-S2 are Coupregulated with SOX2 and OCT4 in Esophageal Squamous Cell Carcinoma

Identification of linc-NeD125, a novel long non coding RNA that hosts miR-125b-1 and negatively controls proliferation of human neuroblastoma cells

Epigenetic setting and reprogramming for neural cell fate determination and differentiation

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