The VMAT-2 inhibitor tetrabenazine alters effort-related decision making as measured by the T-maze barrier choice task: reversal with the adenosine A2A antagonist MSX-3 and the catecholamine uptake blocker bupropion

Yohn, Samantha E.; Thompson, Christian; Randall, Patrick A.; Lee, Christie A.; Müller, Christian; Baqi, Younis; Correa, Mercè; Salamone, John D.

doi:10.1007/s00213-014-3766-0

Cited by 85 publications

(85 citation statements)

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“…Although classical stimulant medications that increase DA release and/or block DA reuptake increase motivation in rodent models Yohn et al, 2015), they have demonstrated only limited efficacy in chronically treating fatigue and other DA-related symptoms in trials for patients with cancer and other medical illnesses that are associated with inflammation (Bruera et al, 2013;Butler et al, 2007;Escalante et al, 2014;Gong et al, 2014;Mar Fan et al, 2008;Moraska et al, 2010;Pucci et al, 2007;Ruddy et As stimulants act to increase DA release and block DAT function to increase synaptic levels of available DA, these drugs may not provide long-term efficacy in the context of inflammation. As described in detail in the section 'Mechanisms of inflammation effects on dopamine synthesis and release' above, although some evidence exists that inflammation may reduce DA packaging and/or release, and decrease DA receptor signaling, the primary mechanism by which inflammation may impact DA transmission is by decreasing DA synthesis, which would lend to only a limited supply of available vesicular or cytosolic DA on which stimulants may act.…”

Section: Potential Therapeutic Targets For Inflammation Effects On Damentioning

confidence: 99%

“…For instance, VMAT2 activity can be increased with the small molecule trkB agonist, 7,8-dihydroxyflavone, which was neuroprotective in a rodent model of PD (Jang et al, 2010). In addition to compounds that may increase DA availability and release, adenosine (A2A) receptor antagonists, which are thought to facilitate the activation of DA D2 receptors, are efficacious in reversing decreased effort-based sucrose consumption after DA depletion with tetrabenazine (a vesicular monoamine transporter inhibitor) and after peripheral administration of IL-1β in rats (Chen et al, 2001;Collins et al, 2010;Nunes et al, 2014;Xie et al, 2009;Yohn et al, 2015). The DA receptor agonist, pramipexole, has been shown to block endotoxin-induced degeneration of nigrostriatal DA cells (Iravani et al, 2008), and has also demonstrated the efficacy in unipolar and bipolar patients with treatment-resistant depression (Cassano et al, 2004;Cusin et al, 2013;Fawcett et al, 2016;Franco-Chaves et al, 2013).…”

Section: Strategies To Facilitate Da Packaging and Release Or Da Recementioning

confidence: 99%

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Inflammation Effects on Motivation and Motor Activity: Role of Dopamine

Felger

Treadway

2016

Neuropsychopharmacol

286

237

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Motivational and motor deficits are common in patients with depression and other psychiatric disorders, and are related to symptoms of anhedonia and motor retardation. These deficits in motivation and motor function are associated with alterations in corticostriatal neurocircuitry, which may reflect abnormalities in mesolimbic and mesostriatal dopamine (DA). One pathophysiologic pathway that may drive changes in DAergic corticostriatal circuitry is inflammation. Biomarkers of inflammation such as inflammatory cytokines and acute-phase proteins are reliably elevated in a significant proportion of psychiatric patients. A variety of inflammatory stimuli have been found to preferentially target basal ganglia function to lead to impaired motivation and motor activity. Findings have included inflammation-associated reductions in ventral striatal neural responses to reward anticipation, decreased DA and DA metabolites in cerebrospinal fluid, and decreased availability, and release of striatal DA, all of which correlated with symptoms of reduced motivation and/or motor retardation. Importantly, inflammation-associated symptoms are often difficult to treat, and evidence suggests that inflammation may decrease DA synthesis and availability, thus circumventing the efficacy of standard pharmacotherapies. This review will highlight the impact of administration of inflammatory stimuli on the brain in relation to motivation and motor function. Recent data demonstrating similar relationships between increased inflammation and altered DAergic corticostriatal circuitry and behavior in patients with major depressive disorder will also be presented. Finally, we will discuss the mechanisms by which inflammation affects DA neurotransmission and relevance to novel therapeutic strategies to treat reduced motivation and motor symptoms in patients with high inflammation.

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Section: Potential Therapeutic Targets For Inflammation Effects On Damentioning

confidence: 99%

Section: Strategies To Facilitate Da Packaging and Release Or Da Recementioning

confidence: 99%

Inflammation Effects on Motivation and Motor Activity: Role of Dopamine

Felger

Treadway

2016

Neuropsychopharmacol

286

237

View full text Add to dashboard Cite

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“…Across multiple paradigms, low doses of DA antagonists and accumbens DA depletions reduce the tendency to work for high reward options and increase selection of low reward choices Correa 2002, 2012;Salamone et al, 2003Salamone et al, , 2007Floresco et al, 2008;Mai et al, 2012;Randall et al, 2012;Hosking et al, 2015). Recent studies have shown that reduced selection of high-effort alternatives in rodents is induced by manipulations associated with depression, including stress (Shafiei et al, 2012), proinflammatory cytokine administration , and injections of the vesicular monoamine transporter-type 2 (VMAT-2) inhibitor tetrabenazine (TBZ; Nunes et al, 2013;Randall et al, 2014;Yohn et al, 2015). TBZ induces depressive symptoms including fatigue in humans (Frank 2010), and recent studies show that this drug shifts choice behavior from high effort to low effort options at doses that do not impair intake of or preference for solid foods or sucrose, hedonic reactivity to sucrose, reference memory, or discrimination of reward magnitude (Nunes et al, 2013;Randall et al, 2014;Pardo et al, 2015;Yohn et al, 2015).…”

Section: Introductionmentioning

confidence: 98%

“…Processes involved in activational aspects of motivation promote the instigation and maintenance of behavior, increase energy expenditure, and facilitate the exertion of effort to overcome obstacles that separate organisms from significant stimuli Correa, 2002, 2012;Yohn et al, 2015). Motivational dysfunctions related to behavioral activation are probably the most common psychiatric symptoms in general medicine (Demyttenaere et al, 2005); symptoms such as anergia, fatigue, psychomotor retardation, or apathy, are frequently observed in people with depression, Parkinsonism, and other disorders (Demyttenaere et al, 2005;Fava et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

“…4 instrumental actions leading to more highly valued reinforcers vs. low effort options leading to less valued reinforcers. In rodents, a variety of tasks have been used to assess effort-related decision making, including operant tasks that offer animals choices between lever pressing for a more preferred food on ratio schedules vs. simply approaching and consuming a less preferred reinforcer (Salamone et al, 2002(Salamone et al, , 2007Schweimer et al, 2005;Randall et al, 2012), effort discounting (Floresco et al, 2008;Hosking et al, 2015), and a T-maze barrier climbing task (Mott et al, 2009;Mai et al, 2012;Yohn et al, 2015). Accumbens dopamine (DA) is involved in regulating energy expenditure, behavioral activation, vigor and exertion of physical effort in motivated behavior Correa, 2002, 2012;Robbins and Everitt, 2007;Mai et al, 2012;McGinty et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

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Not All Antidepressants Are Created Equal: Differential Effects of Monoamine Uptake Inhibitors on Effort-Related Choice Behavior

Yohn

Collins

Contreras-Mora

et al. 2015

Neuropsychopharmacol

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Motivated behavior can be characterized by behavioral activation and high work output. Moreover, people with depression and other disorders show effort-related motivational symptoms, such as anergia, psychomotor retardation, and fatigue. Effort-based decision making is studied using tasks offering choices between high effort options leading to highly valued reinforcers vs low effort/low reward options, and such tasks could be useful as animal models of motivational symptoms. In the present studies the effort-related effects of the vesicular monoamine transport (VMAT-2) inhibitor tetrabenazine (TBZ) were investigated. TBZ blocks vesicular storage and also produces depressive symptoms in humans. Moreover, TBZ alters effort-based choice in rats, biasing animals toward low effort alternatives. The present studies investigated the ability of acute administration of various monoamine uptake inhibitors to reverse the effects of TBZ. Effort-related effects of TBZ were attenuated by the catecholamine uptake inhibitor and antidepressant bupropion, and this effect of bupropion was reversed by either D1 or D2 family antagonism. The effort-related effects of TBZ were also attenuated by the selective dopamine uptake blocker GBR12909. The 5-HT uptake inhibitor fluoxetine and the norepinephrine uptake inhibitor desipramine failed to reverse the effects of TBZ, and higher doses of these drugs, given alone or in combination with TBZ, led to further behavioral impairments. These results indicate that drugs acting on dopamine transmission are relatively effective at reversing the effort-related effects of TBZ, and are consistent with the hypothesis that drugs that enhance dopamine transmission may be effective at treating effort-related psychiatric symptoms in humans.

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Behavioral changes induced through adenosine A2A receptor ligands in a rat depression model induced by olfactory bulbectomy

et al. 2018

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BackgroundMajor depressive disorders are characterized by their severity and long‐lasting symptoms, which make such disorders highly disabling illnesses. Unfortunately, 50% of major depressive patients experience relapses, perhaps partly because drug research has been performed only in animal models that screen for antidepressant drugs that appear to only ameliorate acute depression symptoms. The bilateral olfactory bulbectomy (OBX) animal model presents the advantage of mimicking the symptoms of chronic depression by means of brain surgery. Adenosine purinergic receptors A2A (A2AR) have been the target of interest in the field of psychiatric diseases. This study aimed to show which A2A receptor ligands exert antidepressive‐like effects in the OBX rat model.MethodsForty Sprague‐Dawley male rats were divided into four groups: control, OBX + vehicle, OBX + ZM 241385, and OBX + adenosine groups. Pharmacological treatment was administered for 14 days, and the rats were examined via the forced swim test (FST), open field test (OFT), and sucrose preference test (SPT).ResultsThe OBX + ZM 241385 group exhibited decreased immobility time in the FST, decreased isolation time in the OFT, and reversed anhedonia behavior in the SPT compared to the vehicle group. However, no significant differences for adenosine treatment were found.Conclusions ZM 241385 administration (2 mg/kg i.p.) restored behavioral changes associated with OBX‐induced depression.

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The VMAT-2 inhibitor tetrabenazine alters effort-related decision making as measured by the T-maze barrier choice task: reversal with the adenosine A2A antagonist MSX-3 and the catecholamine uptake blocker bupropion

Cited by 85 publications

References 93 publications

Inflammation Effects on Motivation and Motor Activity: Role of Dopamine

Inflammation Effects on Motivation and Motor Activity: Role of Dopamine

Not All Antidepressants Are Created Equal: Differential Effects of Monoamine Uptake Inhibitors on Effort-Related Choice Behavior

Behavioral changes induced through adenosine A2A receptor ligands in a rat depression model induced by olfactory bulbectomy

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