The histone deacetylase inhibitor sodium butyrate decreases excessive ethanol intake in dependent animals

Simon-O'Brien, Emmanuelle; Alaux‐Cantin, Stéphanie; Warnault, Vincent; Buttolo, Romain; Naassila, Mickaël; Vilpoux, Catherine

doi:10.1111/adb.12161

Cited by 69 publications

(79 citation statements)

References 50 publications

(76 reference statements)

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“…(Palmisano and Pandey, 2017, Kirpich et al, 2013) For example, alcohol craving is associated with brain H3ac deacetylation with a concurrent increase in brain HDAC expression (Palmisano and Pandey, 2017) that can be reversed with administration of oral sodium butyrate. (Simon-O’Brien et al, 2014, Legastelois et al, 2013) Indeed, in the current study H3ac at the Notch1 locus was deacetylated resulting in Notch1 suppression in alcohol-fed mice as shown by ChiP-PCR (Figure 6D). In fact, the Clever’s lab recommends the addition of the HDAC inhibitor valproic acid as a way to activate Notch1 signaling in colonic organoids (Yin et al, 2014) with other studies also demonstrating that HDACi activate Notch1 signaling.…”

Section: Discussionsupporting

confidence: 55%

Alcohol Feeding in Mice Promotes Colonic Hyperpermeability and Changes in Colonic Organoid Stem Cell Fate

Forsyth

Shaikh

Bishehsari

et al. 2017

Alcoholism Clin & Exp Res

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Background Alcohol increases intestinal permeability to pro-inflammatory microbial products that promote liver disease, even after a period of sobriety. We sought to test the hypothesis that alcohol affects intestinal stem cells using an in vivo model and ex vivo organoids generated from jejunum and colon from mice fed chronic alcohol. Methods Mice were fed a control or an alcohol diet. Intestinal permeability, liver steatosis/inflammation, and stool short chain fatty acids (SCFA) were measured. Jejunum and colon organoids and tissue were stained for stem cell, cell lineage, and apical junction markers with assessment of mRNA by PCR and RNA-seq. ChIP-PCR analysis was carried out for Notch1 using an antibody specific for acetylated histone 3. Results Alcohol-fed mice exhibited colonic (but not small intestinal) hyperpermeability, steatohepatitis and decreased butyrate/total SCFA ratio in stool. Stem cell, cell lineage, and apical junction marker staining in tissue or organoids from jejunum tissue were not impacted by alcohol. Only chromogranin A (Chga) was increased in jejunum organoids by qPCR. However, colon tissue and organoid staining exhibited an alcohol-induced significant decrease in cytokeratin 20+ (Krt20) absorptive lineage enterocytes, a decrease in occludin and E-cadherin apical junction proteins, an increase in Chga, and an increase in the Lgr5 stem cell marker. qPCR revealed an alcohol-induced decrease in colon organoid and tissue Notch1, Hes1, and Krt20 and increased Chga, supporting an alteration in stem cell fate due to decreased Notch1 expression. Colon tissue ChIP-PCR revealed alcohol feeding suppressed Notch1 mRNA expression (via deacetylation of histone H3) and decreased Notch1 tissue staining. Conclusions Data support a model for alcohol-induced colonic hyperpermeability via epigenetic effects on Notch1, and thus Hes1, suppression through a mechanism involving histone H3 deacetylation at the Notch1 locus. This decreased enterocyte and increased enteroendocrine cell colonic stem cell fate and decreased apical junctional proteins leading to hyperpermeability.

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Section: Discussionsupporting

confidence: 55%

Alcohol Feeding in Mice Promotes Colonic Hyperpermeability and Changes in Colonic Organoid Stem Cell Fate

Forsyth

Shaikh

Bishehsari

et al. 2017

Alcoholism Clin & Exp Res

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“…Treatment with TSA was able to attenuate development of anxiety-like behaviors during ethanol withdrawal in rats (Pandey et al, 2008a; You et al, 2014). Interestingly, treatment with HDAC inhibitor, sodium butyrate (NaB) significantly attenuated excessive alcohol intake in dependent rats (Simon-O’Brien et al, 2015). Together, these studies suggest that HDAC inhibitors treatment can restore chromatin remodeling and prevent anxiety-like behaviors and dependent-induced excessive alcohol intake in rats.…”

Section: Epigenetic Mechanisms Of Alcohol Addictionmentioning

confidence: 99%

Epigenetic mechanisms of alcoholism and stress-related disorders

Palmisano

Pandey

2017

Alcohol

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Stress-related disorders, such as anxiety, early life stress and posttraumatic stress disorder appear to be important factors in promoting alcoholism, as alcohol consumption can temporarily attenuate the negative affective symptoms of these disorders. Several molecules involved in signaling pathways may contribute to the neuroadaptation induced during alcohol dependence and stress disorders, and among these, brain-derived neurotrophic factor (BDNF), corticotropin releasing factor (CRF), neuropeptide Y (NPY) and opioid peptides (i.e. nociceptin and dynorphin) are involved in the interaction of stress and alcohol. In fact, alterations in the expression and function of these molecules have been associated with the pathophysiology of stress-related disorders and alcoholism. In recent years, various studies have focused on the epigenetic mechanisms that regulate chromatin architecture thereby modifying gene expression. Interestingly, epigenetic modifications in specific brain regions have been shown to be associated with the neurobiology of psychiatric disorders, including alcoholism and stress. In particular, the enzymes responsible for chromatin remodeling (i.e. histone deacetylases and methyltransferases, DNA methyltransferases) have been identified as common molecular mechanisms for the interaction of stress and alcohol and have become promising therapeutic targets to treat or prevent alcoholism and associated emotional disorders.

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“…Sodium butyrate (NAB; Alfa Aesar, Ward Hill, MA), another HDAC inhibitor, was used in order to further validate that the observed behavioral effects were indeed the result of HDAC inhibition and not another, more rapid effect of VPA administration such as an enhancement in GABAergic signaling. NAB was given IP (600 mg/kg, 1200 mg/kg in physiological saline) to a small subset of animals, but it induced a temporary and extreme ataxia, so systemic use was discontinued, and it was only tested site-specifically (1.32 μg/0.2 μl) (Blank et al, 2014; Heinrichs et al, 2013; Kilgore et al, 2010; Lattal et al, 2007; Mahan et al, 2012; Simon-O'Brien et al, 2015). Finally, Curcumin (Epigentek, Farmingdale, NY, 1.1 μg/0.2 μl) was dissolved in 55% DMSO.…”

Section: Methodsmentioning

confidence: 99%

“…This drug was chosen because it appears to be one of the few, if not only, HAT inhibitors that is currently commercially available that does not have to be dissolved in 100% DMSO. All site-specific injections were given 30 min before social defeat (Simon-O'Brien et al, 2015; Xing et al, 2011) at a total volume of 0.2 μl to limit the spread of the injection.…”

Section: Methodsmentioning

confidence: 99%

Histone deacetylase and acetyltransferase inhibitors modulate behavioral responses to social stress

McCann

Rosenhauer

Jones

et al. 2017

Psychoneuroendocrinology

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Histone acetylation has emerged as a critical factor regulating learning and memory both during and after exposure to stressful stimuli. There are drugs that we now know affect histone acetylation that are already in use in clinical populations. The current study uses these drugs to examine the consequences of acutely increasing or decreasing histone acetylation during exposure to social stress. Using an acute model of social defeat in Syrian hamsters, we systemically and site-specifically administered drugs that alter histone acetylation and measured subsequent behavior and immediate-early gene activity. We found that systemic administration of a histone deacetylase inhibitor enhances social stress-induced behavioral responses in males and females. We also found that systemic administration completely blocks defeat-induced neuronal activation, as measured by Fos-immunoreactivity, in the infralimbic cortex, but not in the amygdala, after a mild social defeat stressor. Lastly, we demonstrated that site-specific administration of histone deacetylase inhibitors in the infralimbic region of the prefrontal cortex, but not in the basolateral amygdala, mimics the systemic effect. Conversely, decreasing acetylation by inhibiting histone acetyltransferases in the infralimbic cortex reduces behavioral responses to defeat. This is the first demonstration that acute pharmacological manipulation of histone acetylation during social defeat alters subsequent behavioral responses in both males and females. These results reveal that even systemic administration of drugs that alter histone acetylation can significantly alter behavioral responses to social stress and highlight the importance of the infralimbic cortex in mediating this effect.

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The histone deacetylase inhibitor sodium butyrate decreases excessive ethanol intake in dependent animals

Cited by 69 publications

References 50 publications

Alcohol Feeding in Mice Promotes Colonic Hyperpermeability and Changes in Colonic Organoid Stem Cell Fate

Alcohol Feeding in Mice Promotes Colonic Hyperpermeability and Changes in Colonic Organoid Stem Cell Fate

Epigenetic mechanisms of alcoholism and stress-related disorders

Histone deacetylase and acetyltransferase inhibitors modulate behavioral responses to social stress

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