Literature DB >> 15800190

Retinoic acid-induced chromatin remodeling of mouse kappa opioid receptor gene.

Sung Wook Park1, M D Mostaqul Huq, Horace H Loh, Li-Na Wei.   

Abstract

The mouse kappa opioid receptor (KOR) gene is constitutively expressed in P19 embryonic stem cells but is first suppressed and reactivated during retinoic acid (RA)-induced neuronal differentiation. However, no RA response element (RARE) can be found in this gene regulatory region. The suppression and reactivation of the KOR gene in this neuronal differentiation model suggested chromatin remodeling occurred on this gene promoter triggered by RA induction. This study asks whether RA induces alteration in the nucleosomal structure of this gene promoter that has no apparent RARE and, if so, how RA remodels chromatin of this promoter. The results revealed two loose nucleosomes, N1 at -44 (3' boundary) from the transcription initiation site and N2 spanning the transcription initiation site, that are relevant to active transcription. RA formed a repressive chromatin configuration of this promoter by compacting nucleosome N1, followed by nucleosome N2 condensation. Chromatin immunoprecipitation assay demonstrated RA induced replacement of the c-Myc/Max complex with the Max/Mad1 complex on the E box located within nucleosome N1, coinciding with reduced Sp1 binding to GC boxes located within nucleosome N2 and recruitment of chromatin remodeling factor Brahma-related gene 1 (BRG-1) to this promoter. Consistently, histone deacetylation, Lys9 methylation, and hypophosphorylation of RNA polymerase II C-terminal domain were detected on this promoter after RA treatment. It is concluded that RA induces KOR gene suppression, as early neuronal differentiation marker, by inducing substitution of c-Myc/Max with Max/Mad on the E box and by BRG-1 involved nucleosome recruitment and chromatin condensation, thereby abolishing Sp1 binding.

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Year:  2005        PMID: 15800190      PMCID: PMC6724898          DOI: 10.1523/JNEUROSCI.0186-05.2005

Source DB:  PubMed          Journal:  J Neurosci        ISSN: 0270-6474            Impact factor:   6.167


  30 in total

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Review 3.  Promoter targeting and chromatin remodeling by the SWI/SNF complex.

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4.  Expression of mu-, kappa- and delta-opioid receptors in P19 mouse embryonal carcinoma cells.

Authors:  H C Chen; L N Wei; H H Loh
Journal:  Neuroscience       Date:  1999       Impact factor: 3.590

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Review 7.  Translating the histone code.

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8.  An intronic Ikaros-binding element mediates retinoic acid suppression of the kappa opioid receptor gene, accompanied by histone deacetylation on the promoters.

Authors:  X Hu; J Bi; H H Loh; L N Wei
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9.  Regulation of mouse kappa opioid receptor gene expression by retinoids.

Authors:  J Bi; X Hu; H H Loh; L N Wei
Journal:  J Neurosci       Date:  2001-03-01       Impact factor: 6.167

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  16 in total

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2.  Distinct subcellular distribution of delta-opioid receptor fused with various tags in PC12 cells.

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3.  Up-regulation of the mu-opioid receptor gene is mediated through chromatin remodeling and transcriptional factors in differentiated neuronal cells.

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Review 4.  κ-opioid receptor/dynorphin system: genetic and pharmacotherapeutic implications for addiction.

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Journal:  Trends Neurosci       Date:  2012-06-16       Impact factor: 13.837

5.  Stress-induced epigenetic regulation of κ-opioid receptor gene involves transcription factor c-Myc.

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Authors:  M D Mostaqul Huq; Nien-Pei Tsai; Pawan Gupta; Li-Na Wei
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7.  Epigenetic regulation of kappa opioid receptor gene in neuronal differentiation.

Authors:  S W Park; Y He; S G Ha; H H Loh; L-N Wei
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8.  Loss of pluripotency in human embryonic stem cells directly correlates with an increase in nuclear zinc.

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9.  Evidence of endogenous mu opioid receptor regulation by epigenetic control of the promoters.

Authors:  Cheol Kyu Hwang; Kyu Young Song; Chun Sung Kim; Hack Sun Choi; Xiao-Hong Guo; Ping-Yee Law; Li-Na Wei; Horace H Loh
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10.  Mu and kappa opioids modulate mouse embryonic stem cell-derived neural progenitor differentiation via MAP kinases.

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Journal:  J Neurochem       Date:  2009-11-06       Impact factor: 5.372

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