Neural substrates underlying effort, time, and risk-based decision making in motivated behavior

Orphan G-protein-coupled receptors (oGPCRs) possess untapped potential for drug discovery. In the brain, oGPCRs are generally expressed at low abundance and their function is understudied. Expression profiling is an essential step to position oGPCRs in brain function and disease, however public databases provide only partial information. Here, we fine-map expression of 78 brain-oGPCRs in the mouse, using customized probes in both standard and supersensitive in situ hybridization. Images are available at http://ogpcr-neuromap.douglas.qc.ca. This searchable database contains over 8000 coronal brain sections across 1350 slides, providing the first public mapping resource dedicated to oGPCRs. Analysis with public mouse (60 oGPCRs) and human (56 oGPCRs) genome-wide datasets identifies 25 oGPCRs with potential to address emotional and/or cognitive dimensions of psychiatric conditions. We probe their expression in postmortem human brains using nanoString, and included data in the resource. Correlating human with mouse datasets reveals excellent suitability of mouse models for oGPCRs in neuropsychiatric research.

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“…4, top right) and are highly studied in preclinical neuroscience research 45–48 . A selection of sections is shown in Fig.…”

Section: Resultsmentioning

confidence: 99%

Expression map of 78 brain-expressed mouse orphan GPCRs provides a translational resource for neuropsychiatric research

et al. 2018

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“…Aging is accompanied by a range of neural alterations in brain systems that mediate intertemporal choice, executive functions, and reward motivation (Bailey et al, 2016; Bickel et al, 2011; Sasse et al, 2017; Shamosh et al, 2008). For example, biochemical, electrophysiological and pharmacological evidence indicates that the normal balance of excitatory and inhibitory signaling within the mPFC is markedly altered with advanced age (Bañuelos et al, 2014; Beas et al, 2017; Carpenter et al, 2016; McQuail et al, 2016).…”

Section: 0 Discussionmentioning

confidence: 99%

“…Such alterations have been linked to impaired working memory and cognitive inflexibility, and could directly account for some proportion of the variance in intertemporal choice inasmuch as working memory and/or cognitive flexibility contribute to the increased ability of aged rats to delay gratification. In addition to these cognitive capacities supported directly by the mPFC, this brain region is highly interconnected with other brain regions implicated in intertemporal choice, cognitive flexibility, and incentive motivation, including the orbitofrontal cortex, ventral striatum, and basolateral amygdala (Bailey et al, 2016; Churchwell et al, 2009; Floresco et al, 2008b; Ghods-Sharifi et al, 2009; Hosking et al, 2014; Ishikawa et al, 2008; Jimura et al, 2013; McClure et al, 2004; Samanez-Larkin et al, 2011; Smith et al, 2016; Stalnaker et al, 2009; Tye and Janak, 2007; Wassum and Izquierdo, 2015; Winstanley et al, 2004). Age-associated shifts in excitatory/inhibitory dynamics within PFC may also influence intertemporal choice by altering interactions with these brain regions that integrate cognitive and motivational variables.…”

Section: 0 Discussionmentioning

confidence: 99%

Decline of prefrontal cortical-mediated executive functions but attenuated delay discounting in aged Fischer 344 × brown Norway hybrid rats

Hernandez

Vetere

Orsini

et al. 2017

Neurobiology of Aging

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Despite the fact that prefrontal cortex (PFC) function declines with age, aged individuals generally show an enhanced ability to delay gratification, as evident by less discounting of delayed rewards in intertemporal choice tasks. The current study was designed to evaluate relationships between two aspects of PFC-dependent cognition (working memory and cognitive flexibility) and intertemporal choice in young (6 mo.) and aged (24 mo.) Fischer 344 x Brown-Norway F1 hybrid rats. Rats were also evaluated for motivation to earn rewards using a progressive ratio task. As previously reported, aged rats showed attenuated discounting of delayed rewards, impaired working memory, and impaired cognitive flexibility compared to young. Among aged rats, greater choice of delayed reward was associated with preserved working memory, impaired cognitive flexibility, and less motivation to work for food. These relationships suggest that age-related changes in PFC and incentive motivation contribute to variance in intertemporal choice within the aged population. Cognitive impairments mediated by PFC are unlikely, however, to fully account for the enhanced ability to delay gratification that accompanies aging.

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“…Neuronal activation during TD was evaluated in CHL1-KO (n=6) and WT controls (n=6) in PrL, OFC-med, OFC-vlat, Acb-core, Acb-shell, DS-med, and DS-lat, regions with relevant roles in decision making (Bailey et al, 2016; Floresco et al, 2008), and particularly in TD (da Costa Araujo et al, 2010). Fig.3 indicates a reliable decrease in neuronal activation (number of cFos+ cells) in CHL1-KO mice relative to WT controls in PrL ( t (10)=5.65, p <0.01), DS-med ( t (10)=4.96, p <0.01) and DS-lat ( t (10)=4.05, p <0.01), but no reliable changes in the other brain regions (all t s(10)<1.63, p >0.05).…”

Section: Resultsmentioning

confidence: 99%

Increased temporal discounting after chronic stress in CHL1-deficient mice is reversed by 5-HT2C agonist Ro 60-0175

2017

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Schizophrenia is a neurodevelopmental disorder in which impaired decision-making and goal-directed behaviors are core features. One of the genes associated with schizophrenia is the Close Homolog of L1 (CHL1); CHL1-deficient mice are considered a model of schizophrenia-like deficits, including sensorimotor gating, interval timing and spatial memory impairments. Here we investigated temporal discounting in CHL1-deficient (KO) mice and their wild-type littermates. Although no discounting differences were found under baseline conditions, CHL1-KO mice showed increased impulsive choice following chronic unpredictable stress (fewer % larger-later choices, and reduced area under the discounting curve). Stressed CHL1-KO mice also showed decreased neuronal activation (number of cFos positive neurons) in the discounting task in the prelimbic cortex and dorsal striatum, areas thought to be part of executive and temporal processing circuits. Impulsive choice alterations were reversed by the 5-HT2C agonist Ro 60-0175. Our results provide evidence for a gene×environment, double-hit model of stress-related decision-making impairments, and identify CHL1-deficient mice as a mouse model for these deficits in regard to schizophrenia-like phenotypes.

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Neural substrates underlying effort, time, and risk-based decision making in motivated behavior

Cited by 106 publications

References 204 publications

Expression map of 78 brain-expressed mouse orphan GPCRs provides a translational resource for neuropsychiatric research

Expression map of 78 brain-expressed mouse orphan GPCRs provides a translational resource for neuropsychiatric research

Decline of prefrontal cortical-mediated executive functions but attenuated delay discounting in aged Fischer 344 × brown Norway hybrid rats

Increased temporal discounting after chronic stress in CHL1-deficient mice is reversed by 5-HT2C agonist Ro 60-0175

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