Fatty acid binding protein deletion prevents stress‐induced preference for cocaine and dampens stress‐induced corticosterone levels

Hamilton, John; Marion, Matthew; Figueiredo, Antonio; Clavin, Brendan H.; Deutsch, Dale G.; Kaczocha, Martin; Haj‐Dahmane, Samir; Thanos, Panayotis K.

doi:10.1002/syn.22031

Cited by 13 publications

(6 citation statements)

References 24 publications

(27 reference statements)

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“…Fabp7 was the most highly upregulated DEG in Npas2 mutants across all regions. It regulates fatty acid uptake in astrocytes, sleep (Gerstner et al, 2017) and drug seeking under stressful conditions (Hamilton et al, 2018). Fabp7 is rhythmically expressed throughout the brain (Schnell et al, 2014) and is similarly upregulated in Arntl and Nr1d1 knock-out mice (Schnell et al, 2014;Gerstner and Paschos, 2020).…”

Section: Discussionmentioning

confidence: 99%

Circadian-Dependent and Sex-Dependent Increases in Intravenous Cocaine Self-Administration inNpas2Mutant Mice

et al. 2020

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Substance use disorder (SUD) is associated with disruptions in circadian rhythms. The circadian transcription factor neuronal PAS domain protein 2 (NPAS2) is enriched in reward-related brain regions and regulates reward, but its role in SU is unclear. To examine the role of NPAS2 in drug taking, we measured intravenous cocaine self-administration (acquisition, dose-response, progressive ratio, extinction, cue-induced reinstatement) in wild-type (WT) and Npas2 mutant mice at different times of day. In the light (inactive) phase, cocaine self-administration, reinforcement, motivation and extinction responding were increased in all Npas2 mutants. Sex differences emerged during the dark (active) phase with Npas2 mutation increasing self-administration, extinction responding, and reinstatement only in females as well as reinforcement and motivation in males and females. To determine whether circulating hormones are driving these sex differences, we ovariectomized WT and Npas2 mutant females and confirmed that unlike sham controls, ovariectomized mutant mice showed no increase in self-administration. To identify whether striatal brain regions are activated in Npas2 mutant females, we measured cocaine-induced DFosB expression. Relative to WT, DFosB expression was increased in D11 neurons in the nucleus accumbens (NAc) core and dorsolateral (DLS) striatum in Npas2 mutant females after dark phase self-administration. We also identified potential target genes that may underlie the behavioral responses to cocaine in Npas2 mutant females. These results suggest NPAS2 regulates reward and activity in specific striatal regions in a sex and time of day (TOD)-specific manner. Striatal activation could be augmented by circulating sex hormones, leading to an increased effect of Npas2 mutation in females.

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Section: Discussionmentioning

confidence: 99%

Circadian-Dependent and Sex-Dependent Increases in Intravenous Cocaine Self-Administration inNpas2Mutant Mice

et al. 2020

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“…Pretreatment with the FABP inhibitor SBFI26 significantly reduced ethanol consumption in mice as FABP5 and FABP7 inhibited the transport of anandamide to fatty acid amide hydrolase and elevated anandamide levels in the mouse brain, thereby increasing the preference and consumption of ethanol [ 163 ]. FABP 5/7 double knockout mice exhibit similar acquisition of cocaine-induced CPP relative to WT mice, whereas these mice do not exhibit stress-induced preference and show decreased levels of serum corticosterone under stress relative to WT mice [ 164 ]. Recent studies have reported that FABP5 knockdown in the adult rat NAc shell with RNA interference via adeno-associated viral vector attenuates cocaine self-administration and modulates the excitability of MSNs in the NAc shell [ 165 ].…”

Section: Involvement Of Lcpufas and The Novel Target Fabp3 In Nicomentioning

confidence: 99%

The Role of CaMKII and ERK Signaling in Addiction

Jia

Kawahata

Cheng

et al. 2021

IJMS

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Nicotine is the predominant addictive compound of tobacco and causes the acquisition of dependence through its interactions with nicotinic acetylcholine receptors and various neurotransmitter releases in the central nervous system. The Ca2+/calmodulin-dependent protein kinase II (CaMKII) and extracellular signal-regulated kinase (ERK) play a pivotal role in synaptic plasticity in the hippocampus. CaMKII is involved in long-term potentiation induction, which underlies the consolidation of learning and memory; however, the roles of CaMKII in nicotine and other psychostimulant-induced addiction still require further investigation. This article reviews the molecular mechanisms and crucial roles of CaMKII and ERK in nicotine and other stimulant drug-induced addiction. We also discuss dopamine (DA) receptor signaling involved in nicotine-induced addiction in the brain reward circuitry. In the last section, we introduce the association of polyunsaturated fatty acids and cellular chaperones of fatty acid-binding protein 3 in the context of nicotine-induced addiction in the mouse nucleus accumbens and provide a novel target for the treatment of drug abuse affecting dopaminergic systems.

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“… Rorick-Kehn et al, 2016 eCB (anandamide) enhancer URB597, Cannabidiol + + ? Gonzalez-Cuevas et al, 2018 Chauvet et al, 2014 ; Hamilton et al, 2018 ; Gonzalez-Cuevas et al, 2018 5-HT-3 antagonist Ondansetron, tropisetron + ? ?…”

Section: Neuropharmacological Targetsmentioning

confidence: 99%

“…Using this approach, they demonstrated that URB597 significantly attenuated YOH-reinstatement of cocaine seeking ( Chauvet et al, 2014 ). Targeting fatty acid binding proteins, which transport AEA intracellularly to FAAH for degradation, is a related strategy to interfere with stress-induced drug seeking ( Hamilton et al, 2018 ).…”

Section: Neuropharmacological Targetsmentioning

confidence: 99%

Anti-stress neuropharmacological mechanisms and targets for addiction treatment: A translational framework

Greenwald

2018

Neurobiology of Stress

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Stress-related substance use is a major challenge for treating substance use disorders. This selective review focuses on emerging pharmacotherapies with potential for reducing stress-potentiated seeking and consumption of nicotine, alcohol, marijuana, cocaine, and opioids (i.e., key phenotypes for the most commonly abused substances). I evaluate neuropharmacological mechanisms in experimental models of drug-maintenance and relapse, which translate more readily to individuals presenting for treatment (who have initiated and progressed). An affective/motivational systems model (three dimensions: valence, arousal, control) is mapped onto a systems biology of addiction approach for addressing this problem. Based on quality of evidence to date, promising first-tier neurochemical receptor targets include: noradrenergic (α1 and β antagonist, α2 agonist), kappa-opioid antagonist, nociceptin antagonist, orexin-1 antagonist, and endocannabinoid modulation (e.g., cannabidiol, FAAH inhibition); second-tier candidates may include corticotropin releasing factor-1 antagonists, serotonergic agents (e.g., 5-HT reuptake inhibitors, 5-HT3 antagonists), glutamatergic agents (e.g., mGluR2/3 agonist/positive allosteric modulator, mGluR5 antagonist/negative allosteric modulator), GABA-promoters (e.g., pregabalin, tiagabine), vasopressin 1b antagonist, NK-1 antagonist, and PPAR-γ agonist (e.g., pioglitazone). To address affective/motivational mechanisms of stress-related substance use, it may be advisable to combine agents with actions at complementary targets for greater efficacy but systematic studies are lacking except for interactions with the noradrenergic system. I note clinically-relevant factors that could mediate/moderate the efficacy of anti-stress therapeutics and identify research gaps that should be pursued. Finally, progress in developing anti-stress medications will depend on use of reliable CNS biomarkers to validate exposure-response relationships.

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Fatty acid binding protein deletion prevents stress‐induced preference for cocaine and dampens stress‐induced corticosterone levels

Cited by 13 publications

References 24 publications

Circadian-Dependent and Sex-Dependent Increases in Intravenous Cocaine Self-Administration inNpas2Mutant Mice

Circadian-Dependent and Sex-Dependent Increases in Intravenous Cocaine Self-Administration inNpas2Mutant Mice

The Role of CaMKII and ERK Signaling in Addiction

Anti-stress neuropharmacological mechanisms and targets for addiction treatment: A translational framework

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