Transcriptional regulation of cholesterol 24-hydroxylase by histone deacetylase inhibitors

Shafaati, Marjan; O’Driscoll, Riona; Björkhem, Ingemar; Meaney, Steve

doi:10.1016/j.bbrc.2008.11.103

Cited by 38 publications

(30 citation statements)

References 24 publications

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“…The 0.12pGL2 promoter reporter construct was transfected in SH-SY5Y cells and 24 h after cells were arising from overexpressing this enzyme in a mouse model of AD ( 9 ). We and others have shown that HDACi are one of the few classes of compounds known to induce CYP46A1 expression ( 10,11 ). In our previous study, we showed that the histone deacetylase inhibitor TSA induced a transient histone hyperacetylation of CYP46A1 promoter, which signifi cantly increased CYP46A1 transcription in SH-SY5Y neuroblastoma cells ( 11 ).…”

Section: Okadaic Acid Inhibits Cyp46a1 Basal Expression In Nt2 Human mentioning

confidence: 99%

Okadaic acid inhibits the trichostatin A-mediated increase of human CYP46A1 neuronal expression in a ERK1/2-Sp3-dependent pathway

Nunes

Moutinho

Milagre

et al. 2012

Journal of Lipid Research

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Section: Okadaic Acid Inhibits Cyp46a1 Basal Expression In Nt2 Human mentioning

confidence: 99%

Okadaic acid inhibits the trichostatin A-mediated increase of human CYP46A1 neuronal expression in a ERK1/2-Sp3-dependent pathway

Nunes

Moutinho

Milagre

et al. 2012

Journal of Lipid Research

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“…This effect was time dependentmRNA levels were reduced during the first 24 hours of treatment but the suppression was lost by 48 hours. In contrast, Shafaati et al reported that in SH-SY5Y neuroblastoma cells, the levels of CYP27A1 mRNA increase by a factor of five following treatment with the same HDAC inhibitor [30]. A possible reason for this discrepancy is that HepG2 cells are known to express a relatively large amount of CYP27A1 mRNA in comparison to SH-SY5Y cells and the basal chromatin architecture may and accessory proteins, including HDACs, are likely to be different and respond differently to the broad acting HDAC inhibitor used in these studies.…”

Section: Cyp27a1mentioning

confidence: 89%

“…In this study they reported that HDAC inhibitor treatment led to an increase in the expression of Cyp46a1 mRNA by approximately ten-fold in primary cultures of mouse cortical neurons. Later contemporaneous studies by Shafaati et al and Nunes et al reported that HDAC inhibition led to a profound upregulation of the mRNA expression of CYP46A1 (over 50-fold) in several different cell systems [30,33]. In addition Shafaati et al also reported that treatment of mice with HDAC inhibitors modestly increased the expression of Cyp46a1 in murine liver [30].…”

Section: Cyp46a1mentioning

confidence: 97%

“…Evidence has also been presented that Hnf-1α and Runt-related transcription factor 2 (Runx2) (which is known to be involved in maintenance of epigenetic bookmarking in the context of bone cell development) may have a role in the expression of this gene [58]. Shafaati et al have described that HDACi treatment led to an increase of Cyp39a1 in the brain with a decrease in hepatic expression [30]. In addition, preliminary data suggests that epigenetic mechanisms may have a role in the observed sexual dimorphism of Cyp39a1 (unpublished observations).…”

Section: Cyp39a1mentioning

confidence: 99%

“…Epigenetic regulators of GROS may have potential as anti-atherosclerotic agents whereby these pathways are enhanced following transcriptional therapy with epigenetic regulators. Theoretically, reduction in CYP7B1 and induction of CYP27A1 would optimize this pathway, and evidence has been presented that HDACi may shift the expression of these genes in this manner, at least under in vitro conditions [30]. Epigenetic regulation of the oxidative pathway for cholesterol removal may thus represent a novel anti-atherosclerotic therapy.…”

Section: Applications Of Epigenetic Regulation Of Gros For Sterol Biomentioning

confidence: 99%

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Emerging Role of Epigenetics in Stroke

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pigenetic mechanisms refer to the complex and interrelated molecular processes that dynamically modulate gene expression and function within every cell in the body. These regulatory systems represent the long-sought-after molecular interfaces that mediate geneϫenvironment interactions. Changes in the epigenome throughout life are responsible not only for controlling normal development, adult homeostasis, and aging but also for mediating responses to injury. Emerging evidence implicates a spectrum of epigenetic processes in the pathophysiology of stroke. In this review, we describe conventional epigenetic mechanisms (including DNA methylation, histone code modifications, nucleosome remodeling, and higher-order chromatin formation) and highlight the emerging roles each of these processes play in the pathobiology of stroke. We suggest that understanding these mechanisms may be important for discovering more sensitive and specific biomarkers for risk, onset, and progression of stroke. In addition, we highlight epigenetic approaches for stroke therapy, including the inhibition of DNA methyltransferase and histone deacetylase enzyme activities. These therapeutic approaches are still in their infancy, but preliminary results suggest that contemporary agents targeting these pathways can regulate the deployment of stress responses that modulate neural cell viability and promote brain repair and functional reorganization. Indeed, these agents even appear to orchestrate sophisticated cognitive functions, including learning and memory.

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Transcriptional regulation of cholesterol 24-hydroxylase by histone deacetylase inhibitors

Cited by 38 publications

References 24 publications

Okadaic acid inhibits the trichostatin A-mediated increase of human CYP46A1 neuronal expression in a ERK1/2-Sp3-dependent pathway

Okadaic acid inhibits the trichostatin A-mediated increase of human CYP46A1 neuronal expression in a ERK1/2-Sp3-dependent pathway

Epigenetic regulation of oxysterol formation

Emerging Role of Epigenetics in Stroke

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