Direct Regulation of Diurnal Drd3 Expression and Cocaine Reward by NPAS2

Ozburn, Angela R.; Falcón, Edgardo; Twaddle, Alan; Nugent, Alexandria L.; Gillman, Andrea G.; Spencer, Sade; Arey, Rachel N.; Mukherjee, Shibani; Lyons‐Weiler, James; Self, David W.; McClung, Colleen A.

doi:10.1016/j.biopsych.2014.07.030

Cited by 80 publications

(126 citation statements)

References 47 publications

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“…For example, while CLOCK is largely expressed across many brain regions, expression of the paralog NPAS2, a circadian transcription factor structurally and functionally similar to CLOCK, is primarily limited to the mammalian forebrain and striatum [19,35,37,38]. Significantly, striatal expression of NPAS2 has been implicated as a modulator of drug reward and addiction [19,39]. Recent work also suggests NPAS2 may drive circadian transcription of genes with important roles in neuronal metabolism and energy homeostasis [40–45].…”

Section: The Cns Circadian Systemmentioning

confidence: 99%

“…Similar impairments of glycolysis either via direct blockade or by preventing lactate transport through MCT1 or MCT2 knockdown reduce the acquisition and maintenance of cocaine conditioned place preference and the number of infusions during cocaine self-administration [23,24]. Intriguingly, NPAS2 knockdown in the NAc also attenuates the acquisition of cocaine conditioned place preference, further suggesting the induction of NPAS2 is important for cocaine conditioned reward[19]. Given these data, we speculate that NPAS2 may be a transcriptional regulator of energy production in the NAc via the induction of Ldha and lactate production necessary for drug-paired contextual conditioning.…”

Section: Circadian Brain Lactate Production and Drug-induced Plasticimentioning

confidence: 99%

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The intertwined roles of circadian rhythmsand neuronal metabolism fueling drug reward and addiction

Freyberg

Logan

2018

Current Opinion in Physiology

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Drug addiction is a highly prevalent and devastating disorder with few effective treatments, resulting in enormous burdens on family and society. The cellular and behavioral effects of drugs of abuse are related to their abilities to elevate synaptic dopamine levels. Midbrain dopaminergic neurons projecting from the ventral tegmental area to the nucleus accumbens play crucial roles in substance-induced neural and behavioral plasticity. Significantly, increasing work suggests that interplay between the brain circadian system and the cellular bioenergetic machinery in these dopamine neurons plays a critical role in mediating the actions of drugs of abuse. Here, we describe recent progress in elucidating the interconnections between circadian and metabolic systems at the molecular and cellular levels and their relationships to modulation of drug reward and addiction.

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Section: The Cns Circadian Systemmentioning

confidence: 99%

Section: Circadian Brain Lactate Production and Drug-induced Plasticimentioning

confidence: 99%

The intertwined roles of circadian rhythmsand neuronal metabolism fueling drug reward and addiction

Freyberg

Logan

2018

Current Opinion in Physiology

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“…First, they demonstrated that Clock Δ 19 -mutant mice, carrying a single point mutation inducing the protein CLOCK, are devoid of any transcriptional activity in all CLOCK-expressing cells, and display increased cocaine-induced conditioned place preference and self-administration when compared to wild-type mice (McClung, Nestler, & Zachariou, 2005; Ozburn, Larson, Self, & McClung, 2012). Most recently, they showed that, when applied specifically within the nucleus accumbens, adeno-associated virus-short hairpin RNA mediating knockdown of the gene Clock does not seem to affect cocaine-induced behaviors, whereas such expression knockdown of the gene Npas2 decreases cocaine-induced conditioned place preference and self-administration (Ozburn et al, 2015). …”

Section: Clock Genes – New Key Players In Aud and Sudsmentioning

confidence: 99%

Clock genes × stress × reward interactions in alcohol and substance use disorders

Perreau-Lenz

Spanagel

2015

Alcohol

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Adverse life events and highly stressful environments have deleterious consequences for mental health. Those environmental factors can potentiate alcohol and drug abuse in vulnerable individuals carrying specific genetic risk factors, hence producing the final risk for alcohol- and substance-use disorders development. The nature of these genes remains to be fully determined, but studies indicate their direct or indirect relation to the stress hypothalamo-pituitary-adrenal (HPA) axis and/or reward systems. Over the past decade, clock genes have been revealed to be key-players in influencing acute and chronic alcohol/drug effects. In parallel, the influence of chronic stress and stressful life events in promoting alcohol and substance use and abuse has been demonstrated. Furthermore, the reciprocal interaction of clock genes with various HPA-axis components, as well as the evidence for an implication of clock genes in stress-induced alcohol abuse, have led to the idea that clock genes, and Period genes in particular, may represent key genetic factors to consider when examining gene × environment interaction in the etiology of addiction. The aim of the present review is to summarize findings linking clock genes, stress, and alcohol and substance abuse, and to propose potential underlying neurobiological mechanisms.

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“…Using FACS, ~30,000 tdTomato+ cells were collected from NAc with minimal tissue processing time (~45 min), providing sufficient RNA and chromatin for downstream analysis. This one day ChIP protocol is an improvement over previous protocols that describe pooling multiple animals (16, 22, 33) and is expected to facilitate epigenetic analysis of neuronal subtypes in a variety of experimental settings.…”

Section: Discussionmentioning

confidence: 99%

“…A recent study utilized BAC transgenic strains along with antibody-mediated tagging of histone modifications to examine how cocaine alters histone modifications in D1R and D2R MSNs (14). Other groups have used antibody-mediated FACS to study gene regulation induced by cocaine (15, 16), opioids (17, 18), and methamphetamine (19) in cellular subtypes. However, while antibody-based approaches allow for selection of a wider array of cell types compared to BAC transgenic strains, they also require fixing cells and have issues with off-target binding by antibodies that may reduce their specificity.…”

Section: Introductionmentioning

confidence: 99%

Chromatin immunoprecipitation and gene expression analysis of neuronal subtypes after fluorescence activated cell sorting

Finegersh

Homanics

2016

Journal of Neuroscience Methods

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Background With advances in cell capture, gene expression can now be studied in neuronal subtypes and single cells; however, studying epigenetic mechanisms that underlie these changes presents challenges. Moreover, chromatin immunoprecipitation (ChIP) protocols optimized for low cell number do not adequately address technical issues and cell loss while preparing tissue for fluorescence activated cell sorting (FACS). Developing a reliable FACS-ChIP protocol without the need for pooling tissue from multiple animals would enable study of epigenetic mechanisms in neuronal subtypes. Methods FACS was used to isolate dopamine 1 receptor (D1R) expressing cells from the nucleus accumbens (NAc) of a commercially available BAC transgenic mouse strain. D1R+ cells were used to study gene expression as well as histone modifications at gene promoters using a novel native ChIP protocol. Results Isolated cells had enrichment of the dopamine 1 receptor (D1R) mRNA and nearly undetectable levels of GFAP and D2R mRNA. ChIP analysis demonstrated the association of activating or repressive histone modifications with highly expressed or silent gene promoters, respectively. Comparison with existing methods: The ChIP protocol developed in this paper enables characterization of histone modifications from ~30,000 FAC-sorted neurons. Conclusions We describe a one day FACS-ChIP protocol that can be applied to epigenetic studies of neuronal subtypes without pooling tissue.

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Direct Regulation of Diurnal Drd3 Expression and Cocaine Reward by NPAS2

Cited by 80 publications

References 47 publications

The intertwined roles of circadian rhythmsand neuronal metabolism fueling drug reward and addiction

The intertwined roles of circadian rhythmsand neuronal metabolism fueling drug reward and addiction

Clock genes × stress × reward interactions in alcohol and substance use disorders

Chromatin immunoprecipitation and gene expression analysis of neuronal subtypes after fluorescence activated cell sorting

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