Dopamine Production in the Caudate Putamen Restores Feeding in Dopamine-Deficient Mice

Szczypka, Mark S.; Kwok, K. H.H.; Brot, Michelle D.; Marck, Brett T.; Matsumoto, Alvin M.; Donahue, Brian A.; Palmiter, Richard D.

doi:10.1016/s0896-6273(01)00319-1

Cited by 317 publications

(257 citation statements)

References 48 publications

(1 reference statement)

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“…Pleasurable subjective pain relief for chronic pain in a phantom limb in a patient was causally induced by effective deep brain stimulation in the PVG/ PAG part of the brainstem. When using MEG to directly measure the concomitant changes in the rest of the brain, a significant change in power was found in the mid-anterior OFC to enhance several aspects of reward (Cardinal et al 2002;Everitt and Robbins 2005;Kelley et al 2002;Kelley et al 2005;Koob and Le Moal 2006;Kringelbach and Berridge 2008;Peciña et al 2006;Robbins and Everitt 2002;Salamone et al 2007;Shizgal et al 2001;Szczypka et al 2001), yet damage to the nucleus accumbens may only subtly impair the hedonic impact or related components of natural rewards such as food (Balleine and Killcross 1994;Parkinson et al 1999;Setlow et al 2002;Whishaw and Kornelsen 1993). Core 'liking' reactions to pleasure may be relatively difficult to abolish absolutely by a single brain lesion or drug, which may be very good in evolutionary terms.…”

Section: Pleasure Coding Versus Causalitymentioning

confidence: 99%

Affective neuroscience of pleasure: reward in humans and animals

2008

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Introduction Pleasure and reward are generated by brain circuits that are largely shared between humans and other animals. Discussion Here, we survey some fundamental topics regarding pleasure mechanisms and explicitly compare humans and animals. Conclusion Topics surveyed include liking, wanting, and learning components of reward; brain coding versus brain causing of reward; subjective pleasure versus objective hedonic reactions; roles of orbitofrontal cortex and related cortex regions; subcortical hedonic hotspots for pleasure generation; reappraisals of dopamine and pleasure-electrode controversies; and the relation of pleasure to happiness.

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Section: Pleasure Coding Versus Causalitymentioning

confidence: 99%

Affective neuroscience of pleasure: reward in humans and animals

2008

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“…Moreover, restoration of tyrosine hydroxylase gene expression using gene therapy was able rescue the deficient feeding behavior in these DA-deficient mice [303]. Using gene therapy to enable DA production within only the caudate putamen restored mouse feeding on regular chow diet, and also normal nest-building behavior, whereas restoration of DA production into the NAc only restored the exploratory behavior [304]. …”

Section: Reviewmentioning

confidence: 99%

“…However, restoration of DA into the NAc in these studies was not sufficient to rescue normal feeding behavior, but this may have been due to an inability to anatomically restore gene expression throughout the entire NAc [304]. Interestingly, when the DA-deficient mice are crossed with obese leptin (Ob/Ob)-deficient mice, the lack of DA blocked the increased feeding behavior normally present in the leptin (Ob/Ob)-deficient mice [305].…”

Section: Reviewmentioning

confidence: 99%

Reward circuitry dysfunction in psychiatric and neurodevelopmental disorders and genetic syndromes: animal models and clinical findings

Dichter

Damiano

Allen

2012

J Neurodevelop Disord

253

207

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This review summarizes evidence of dysregulated reward circuitry function in a range of neurodevelopmental and psychiatric disorders and genetic syndromes. First, the contribution of identifying a core mechanistic process across disparate disorders to disease classification is discussed, followed by a review of the neurobiology of reward circuitry. We next consider preclinical animal models and clinical evidence of reward-pathway dysfunction in a range of disorders, including psychiatric disorders (i.e., substance-use disorders, affective disorders, eating disorders, and obsessive compulsive disorders), neurodevelopmental disorders (i.e., schizophrenia, attention-deficit/hyperactivity disorder, autism spectrum disorders, Tourette’s syndrome, conduct disorder/oppositional defiant disorder), and genetic syndromes (i.e., Fragile X syndrome, Prader–Willi syndrome, Williams syndrome, Angelman syndrome, and Rett syndrome). We also provide brief overviews of effective psychopharmacologic agents that have an effect on the dopamine system in these disorders. This review concludes with methodological considerations for future research designed to more clearly probe reward-circuitry dysfunction, with the ultimate goal of improved intervention strategies.

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“…Besides mental retardation, fragile X individuals can have seizures, attention deficit, hyperactivity, anxiety, and symptoms associated with autism (Chen and Toth, 2001;Consortium, 1994 Here we report that in the mouse model of fragile X hyperactivity is maternally transmitted, at least partly, while seizures, reduced startle and increased prepulse inhibition are strictly Mendelian traits. Since hyperactivity has been linked to low tonic stimulation of inhibitory dopamine (DA) D2 autoreceptors and consecutively to high phasic DA activity in the striatum (Grace, 2001;Koob et al, 1981;Koob and Swerdlow, 1988;Szczypka et al, 2001), we tested the function of these receptors by quinpirole, a D2 receptor preferring drug (Cory-Slechta et al, 1996; Two cohorts of animals were tested and since they were not statistically different from each other the data from the two experiments were combined. Main effect ANOVA showed both a maternal and offspring genotype effect (see in the Results and Discussion section).…”

Section: Introductionmentioning

confidence: 99%

Wild-Type Male Offspring of fmr-1+/− Mothers Exhibit Characteristics of the Fragile X Phenotype

Zupan

Tóth

2008

Neuropsychopharmacol

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Fragile X syndrome is an X-linked disorder caused by the inactivation of the FMR-1 gene with symptoms ranging from impaired cognitive functions to seizures, anxiety, sensory abnormalities, and hyperactivity. Males are more severely affected than heterozygote (H) females, who, as carriers, have a 50% chance of transmitting the mutated allele in each pregnancy. fmr-1 knockout (KO) mice reproduce fragile X symptoms, including hyperactivity, seizures, and abnormal sensory processing. In contrast to the expectation that wild-type (WT) males born to H (fmr-1 + /À ) mothers (H4WT) are behaviorally normal and indistinguishable from WT males born to WT mothers (WT4WT); here, we show that H4WT offspring are more active than WT4WT offspring and that their hyperactivity is similar to male KO mice born to H or KO (fmr-1 À/À ) mothers (H4KO/KO4KO). H4WT mice, however, do not exhibit seizures or abnormal sensory processing. Consistent with their hyperactivity, the effect of the D2 agonist quinpirole is reduced in H4WT as well as in H4KO and KO4KO mice compared to WT4WT offspring, suggesting a diminished feedback inhibition of dopamine release. Our data indicate that some aspects of hyperactivity and associated dopaminergic changes in 'fragile X' mice are a maternal fmr-1 genotype rather than an offspring fmr-1 genotype effect.

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Dopamine Production in the Caudate Putamen Restores Feeding in Dopamine-Deficient Mice

Cited by 317 publications

References 48 publications

Affective neuroscience of pleasure: reward in humans and animals

Affective neuroscience of pleasure: reward in humans and animals

Reward circuitry dysfunction in psychiatric and neurodevelopmental disorders and genetic syndromes: animal models and clinical findings

Wild-Type Male Offspring of fmr-1+/− Mothers Exhibit Characteristics of the Fragile X Phenotype

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