2019
DOI: 10.1111/gbb.12600
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Nuclear transcriptional changes in hypothalamus of Pomc enhancer knockout mice after excessive alcohol drinking

Abstract: Persistent alterations of proopiomelanocortin (Pomc) and mu‐opioid receptor (Oprm1) activity and stress responses after alcohol are critically involved in vulnerability to alcohol dependency. Gene transcriptional regulation altered by alcohol may play important roles. Mice with genome‐wide deletion of neuronal Pomc enhancer1 (nPE1−/−), had hypothalamic‐specific partial reductions of beta‐endorphin and displayed lower alcohol consumption, compared to wildtype littermates (nPE1+/+). We used RNA‐Seq to measure st… Show more

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Cited by 10 publications
(5 citation statements)
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References 55 publications
(172 reference statements)
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“…In regional analyses between the two time points, we found no significant DMRs, although some genes known to be associated with inflammatory and immune processes ( MIR637 , RUNX3 , AVPI1 , MCF2L , FOXK2 , POU6F1 ) were noted. Moreover, FAM124B is related to anorexia nervosa [ 29 ], and AVPI1 is associated with alcohol dependence [ 26 ]. In the regional analyses including clinical symptoms variation as a covariate, we identified several significant DMRs annotated in notable genes.…”
Section: Discussionmentioning
confidence: 99%
“…In regional analyses between the two time points, we found no significant DMRs, although some genes known to be associated with inflammatory and immune processes ( MIR637 , RUNX3 , AVPI1 , MCF2L , FOXK2 , POU6F1 ) were noted. Moreover, FAM124B is related to anorexia nervosa [ 29 ], and AVPI1 is associated with alcohol dependence [ 26 ]. In the regional analyses including clinical symptoms variation as a covariate, we identified several significant DMRs annotated in notable genes.…”
Section: Discussionmentioning
confidence: 99%
“…In another study, voluntary consumption was reduced in β-endorphin knockout mice with a stronger reduction in female mice [47]. Recently, a mouse line with a genome-wide deletion of neuronal Pomc enhancer 1 was generated [127]. This deletion reduces specifically βendorphin levels in the hypothalamus and decreases significantly alcohol consumption in two alcohol drinking paradigms: drinking in the dark and intermittent access [127].…”
Section: Morsmentioning
confidence: 99%
“…Conditional MOR deletion in GABAergic forebrain neurons using a Dlx5/6-Cre driver line (Cre expressed in GABAergic neurons [125] crossed with floxed Oprm1 mice) diminished voluntary alcohol drinking and alcohol rewarding properties [126]. Endogenous peptides binding to MORs such as β-endorphin and his precursor proopiomelanocortin (POMC) have also been implicated in alcohol use and abuse disorders [121,127,128]. Specifically, β-endorphin heterozygote knockout mice showed an increased voluntary alcohol consumption in a two-bottle choice paradigm [46].…”
Section: Morsmentioning
confidence: 99%
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“…Researchers often choose the hypothalamus to analyze transcriptomic changes after exposure to various stressors: heat stress for 24 h [ 9 ] or for 14 days [ 10 , 11 ], social conflict (within 20 days) [ 12 ], alcohol consumption [ 13 ], short-term starvation [ 14 ], and repeated homotypic stress [ 15 ]. The hypothalamic transcriptome has also been investigated when studying the molecular mechanisms of blood pressure regulation.…”
Section: Introductionmentioning
confidence: 99%