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18. Reward-Mediated, Model-Free Reinforcement-Learning Mechanisms in Pavlovian and Instrumental Tasks Are Related.

Author

Afshar, Neema Moin, Cinotti, François, Martin, David, Khamassi, Mehdi, Calu, Donna J., Taylor, Jane R., and Groman, Stephanie M.

Subjects
OPERANT conditioning, OPERANT behavior, REWARD (Psychology), REINFORCEMENT learning, ASSOCIATIVE learning
Abstract

Model-free and model-based computations are argued to distinctly update action values that guide decision-making processes. It is not known, however, if these model-free and model-based reinforcement learning mechanisms recruited in operationally based instrumental tasks parallel those engaged by pavlovian-based behavioral procedures. Recently, computational work has suggested that individual differences in the attribution of incentive salience to reward predictive cues, that is, sign- and goaltracking behaviors, are also governed by variations in model-free and model-based value representations that guide behavior. Moreover, it is not appreciated if these systems that are characterized computationally using model-free and model-based algorithms are conserved across tasks for individual animals. In the current study, we used a within-subject design to assess sign-tracking and goal-tracking behaviors using a pavlovian conditioned approach task and then characterized behavior using an instrumental multistage decision-making (MSDM) task in male rats. We hypothesized that both pavlovian and instrumental learning processes may be driven by common reinforcement-learning mechanisms. Our data confirm that sign-tracking behavior was associated with greater reward-mediated, model-free reinforcement learning and that it was also linked to model-free reinforcement learning in the MSDM task. Computational analyses revealed that pavlovian model-free updating was correlated with model-free reinforcement learning in the MSDM task. These data provide key insights into the computational mechanisms mediating associative learning that could have important implications for normal and abnormal states. [ABSTRACT FROM AUTHOR]

Published
2023
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24. The effects of fatty acid amide hydrolase inhibition and monoacylglycerol lipase inhibition on habit formation in mice.

Author

Gianessi, Carol A., Groman, Stephanie M., and Taylor, Jane R.

Subjects
*CANNABINOID receptors, *FATTY acids, *LIPASES, *HABIT, *SYNTHETIC marijuana
Abstract

Emerging data indicate that endocannabinoid signaling is critical to the formation of habitual behavior. Previous work demonstrated that antagonism of cannabinoid receptor type 1 (CB1R) with AM251 during operant training impairs habit formation, but it is not known if this behavioral effect is specific to disrupted signaling of the endocannabinoid ligands anandamide or 2‐arachidonoyl glycerol (2‐AG). Here, we used selective pharmacological compounds during operant training to determine the impact of fatty acid amide hydrolase (FAAH) inhibition to increase anandamide (and other n‐acylethanolamines) or monoacylglycerol lipase (MAGL) inhibition to increase 2‐AG levels on the formation of habitual behaviors in mice using a food‐reinforced contingency degradation procedure. We found, contrary to our hypothesis, that inhibition of FAAH and of MAGL disrupted the formation of habits. Next, AM251 was administered during training to verify that impaired habit formation could be assessed using contingency degradation. AM251‐exposed mice responded at lower rates during training and at higher rates in the test. To understand the inconsistency with published data, we performed a proof‐of‐principle dose–response experiment to compare AM251 in our vehicle‐solution to the published vehicle‐suspension on response rates. We found consistent reductions in response rate with increasing doses of AM251 in solution and an inconsistent dose–response relationship with AM251 in suspension. Together, our data suggest that further characterization of the role of CB1R signaling in the formation of habitual responding is warranted and that augmenting endocannabinoids may have clinical utility for prophylactically preventing aberrant habit formation such as that hypothesized to occur in substance use disorders. [ABSTRACT FROM AUTHOR]

Published
2022
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25. Unlocking the reinforcement-learning circuits of the orbitofrontal cortex.

Author

Groman, Stephanie M., Lee, Daeyeol, and Taylor, Jane R.

Abstract

Neuroimaging studies have consistently identified the orbitofrontal cortex (OFC) as being affected in individuals with neuropsychiatric disorders. OFC dysfunction has been proposed to be a key mechanism by which decision-making impairments emerge in diverse clinical populations, and recent studies employing computational approaches have revealed that distinct reinforcement-learning mechanisms of decision-making differ among diagnoses. In this perspective, we propose that these computational differences may be linked to select OFC circuits and present our recent work that has used a neurocomputational approach to understand the biobehavioral mechanisms of addiction pathology in rodent models. We describe how combining translationally analogous behavioral paradigms with reinforcement-learning algorithms and sophisticated neuroscience techniques in animals can provide critical insights into OFC pathology in biobehavioral disorders. [ABSTRACT FROM AUTHOR]

Published
2021
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26. Introducing the PLOS ONE Collection on the neuroscience of reward and decision making.

Author

Groman, Stephanie M., Ikemoto, Satoshi, Rushworth, Matthew, Taylor, Jane R., and Whelan, Robert

Subjects
*DECISION making, *FORECASTING, *BEHAVIORAL neuroscience, *COLLECTIONS, *NEUROSCIENCES
Abstract

The survival of an organism depends on the ability to make adaptive decisions to achieve the needs of the organism: where to get food, who to mate with, and how to evade predators. Decision-making is a term used to describe a collection of behavioral and/or computational functions that guide the selection of an option amongst a set of alternatives. Some of these functions may include calculating the costs and benefits of a particular action, evaluating differences in value of each of the alternative outcomes and the likelihood of receiving a particular outcome, using past experiences to generate predictions or expectations about action-outcome associations, and/or integration of past experiences to make novel inferences that can be used in new environments. There is considerable interest in understanding the neurobiological mechanisms that mediate these decision-making functions and recent advances in behavioral approaches, neuroscience techniques, and neuroimaging measures have begun to develop mechanistic links between biology, reward, and decision making. This multidisciplinary work holds great promise for elucidating the biological mechanisms mediating decision-making deficits in normal and abnormal states. The multidisciplinary studies included in this Collection provide new insights into the neuroscience of decision making and reward. [ABSTRACT FROM AUTHOR]

Published
2020
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27. Reinforcement Learning during Adolescence in Rats.

Author

Afshar, Neema Moin, Keip, Alex J., Taylor, Jane R., Lee, Daeyeol, and Groman, Stephanie M.

Subjects
REINFORCEMENT learning, ADOLESCENCE, RATS, NEURAL development, PUERPERIUM, COMPUTER adaptive testing
Abstract

The most dynamic period of postnatal brain development occurs during adolescence, the period between childhood and adulthood. Neuroimaging studies have observed morphologic and functional changes during adolescence, and it is believed that these changes serve to improve the functions of circuits that underlie decision-making. Direct evidence in support of this hypothesis, however, has been limited because most preclinical decision-making paradigms are not readily translated to humans. Here, we developed a reversal-learning protocol for the rapid assessment of adaptive choice behavior in dynamic environments in rats as young as postnatal day 30. A computational framework was used to elucidate the reinforcementlearning mechanisms that change in adolescence and into adulthood. Using a cross-sectional and longitudinal design, we provide the first evidence that value-based choice behavior in a reversal-learning task improves during adolescence in male and female Long-Evans rats and demonstrate that the increase in reversal performance is due to alterations in value updating for positive outcomes. Furthermore, we report that reversal-learning trajectories in adolescence reliably predicted reversal performance in adulthood. This novel behavioral protocol provides a unique platform for conducting biological and systems-level analyses of the neurodevelopmental mechanisms of decision-making. [ABSTRACT FROM AUTHOR]

Published
2020
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28. Medial Nucleus Accumbens Projections to the Ventral Tegmental Area Control Food Consumption.

Author

Bond, Colin W., Trinko, Richard, Foscue, Ethan, Furman, Kara, Groman, Stephanie M., Taylor, Jane R., and DiFeone, Ralph J.

Subjects
NUCLEUS accumbens, FOOD consumption, FOOD supply, REINFORCEMENT learning, MESENCEPHALON
Abstract

Decades of research have shown that the NAc is a critical region influencing addiction, mood, and food consumption through its effects on reinforcement learning, motivation, and hedonic experience. Pharmacological studies have demonstrated that inhibition of the NAc shell induces voracious feeding, leading to the hypothesis that the inhibitory projections that emerge from the NAc normally act to restrict feeding. While much of this work has focused on projections to the lateral hypothalamus, the role of NAc projections to the VTA in the control food intake has been largely unexplored. Using a retrograde viral labeling technique and real-time monitoring of neural activity with fiber photometry, we find that medial NAc shell projections to the VTA (mNAc--»VTA) are inhibited during food-seeking and food consumption in male mice. We also demonstrate that this circuit bidirectionally controls feeding: optogenetic activation of NAc projections to the VTA inhibits food-seeking and food intake (in both sexes), while optogenetic inhibition of this circuit potentiates food-seeking behavior. Additionally, we show that activity of the NAc to VTA pathway is necessary for adaptive inhibition of food intake in response to external cues. These data provide new insight into NAc control over feeding in mice, and contribute to an emerging literature elucidating the role of inhibitory midbrain feedback within the mesolimbic circuit. [ABSTRACT FROM AUTHOR]

Published
2020
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29. Endocannabinoid contributions to alcohol habits and motivation: Relevance to treatment.

Author

Gianessi, Carol A., Groman, Stephanie M., Thompson, Summer L., Jiang, Ming, Stelt, Mario, Taylor, Jane R., and van der Stelt, Mario

Subjects
*ALCOHOLISM, *COMPULSIVE behavior, *LIPASE inhibitors, *CANNABINOID receptors, *RODENT behavior, *DRUG metabolism, *RESEARCH, *GLYCERIDES, *MOTIVATION (Psychology), *ANIMAL experimentation, *HETEROCYCLIC compounds, *RESEARCH methodology, *NEUROTRANSMITTERS, *HABIT, *CELL receptors, *MEDICAL cooperation, *EVALUATION research, *PIPERIDINE, *COMPARATIVE studies, *ALCOHOL drinking, *DRUGS, *RESEARCH funding, *ARACHIDONIC acid, *ESTERASES, *ETHANOL, *CENTRAL nervous system depressants, *MICE, *PHARMACODYNAMICS, *CHEMICAL inhibitors
Abstract

Individuals with alcohol use disorder exhibit compulsive habitual behaviors that are thought to be, in part, a consequence of chronic and persistent use of alcohol. The endocannabinoid system plays a critical role in habit learning and in ethanol self-administration, but the role of this neuromodulatory system in the expression of habitual alcohol seeking is unknown. Here, we investigated the role of the endocannabinoid system in established alcohol habits using contingency degradation in male C57BL/6 mice. We found that administration of the novel diacyl glycerol lipase inhibitor DO34, which decreases the biosynthesis of the endocannabinoid 2-arachidonoyl glycerol (2-AG), reduced habitual responding for ethanol and ethanol approach behaviors. Moreover, administration of the endocannabinoid transport inhibitor AM404 or the cannabinoid receptor type 1 antagonist AM251 produced similar reductions in habitual responding for ethanol and ethanol approach behaviors. Notably, AM404 was also able to reduce ethanol seeking and consumption in mice that were insensitive to lithium chloride-induced devaluation of ethanol. Conversely, administration of JZL184, a monoacyl glycerol lipase inhibitor that increases levels of 2-AG, increased motivation to respond for ethanol on a progressive ratio schedule of reinforcement. These results demonstrate an important role for endocannabinoid signaling in the motivation to seek ethanol, in ethanol-motivated habits, and suggest that pharmacological manipulations of endocannabinoid signaling could be effective therapeutics for treating alcohol use disorder. [ABSTRACT FROM AUTHOR]

Published
2020
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31. Low circulating levels of bisphenol-A induce cognitive deficits and loss of asymmetric spine synapses in dorsolateral prefrontal cortex and hippocampus of adult male monkeys

Author

Elsworth, John D, Jentsch, James D, Groman, Stephanie M, Roth, Robert H, Redmond, D. Eugene, and Leranth, Csaba

Subjects
Male, endocrine system, urogenital system, Dendritic Spines, Pyramidal Cells, Prefrontal Cortex, Air Pollutants, Occupational, Environmental Exposure, Neuropsychological Tests, Article, Microscopy, Electron, Memory, Short-Term, Phenols, Chlorocebus aethiops, Models, Animal, Synapses, Animals, Benzhydryl Compounds, Cognition Disorders, CA1 Region, Hippocampal, hormones, hormone substitutes, and hormone antagonists
Abstract

Bisphenol-A (BPA) is widely used in the manufacture of plastics, epoxy resins, and certain paper products. A majority of the population in the developed world is routinely exposed to BPA from multiple sources and has significant circulating levels of BPA. Although BPA is categorized as an endocrine disruptor with a growing literature on adverse effects, it is uncertain whether cognitive dysfunction is induced in humans by exposure to BPA. The present study examined the impact of BPA in primate brain by exposing adult male vervet monkeys for 4 weeks continuously to circulating levels of BPA that were in the range measured in studies of humans environmentally exposed to BPA. This regimen of exposure to BPA decreased both working memory accuracy and the number of excitatory synaptic inputs on dendritic spines of pyramidal neurons in two brain regions that are necessary for working memory (prefrontal cortex and hippocampus). These observed behavioral and synaptic effects were ameliorated following withdrawal from BPA. As Old World monkeys (e.g., vervets) and humans share some uniquely primate morphological, endocrine, and cognitive traits, this study indicates the potential for significant cognitive disruption following exposure of humans to BPA.

Published
2015

32. Bi‐directional modulation of food habit expression by the endocannabinoid system.

Author

Gianessi, Carol A., Groman, Stephanie M., and Taylor, Jane R.

Subjects
*FOOD habits, *CANNABINOID receptors, *SUBSTANCE-induced disorders, *ACTION theory (Psychology), *NEURAL circuitry
Abstract

The compulsive, habitual behaviors that have been observed in individuals diagnosed with substance use disorders may be due to disruptions in the neural circuits that mediate goal‐directed actions. The endocannabinoid system has been shown to play a critical role in habit learning, but the role of this neuromodulatory system in habit expression is unclear. Here, we investigated the role of the endocannabinoid system in established habitual actions using contingency degradation in male C57BL/6 mice. We found that administration of the endocannabinoid transport inhibitor AM404 reduced habitual responding for food and that antagonism of cannabinoid receptor type 1 (CB1), but not transient receptor potential cation subfamily V (TRPV1), receptors produced a similar reduction in habitual responding. Moreover, pharmacological stimulation of CB1 receptors increased habitual responding for food. Co‐administration of an enzyme inhibitor that selectively increases the endocannabinoid 2‐arachidonoyl glycerol (2‐AG) with AM404 partially restored habitual responding for food. Together, these findings demonstrate an important role for the endocannabinoid system in the expression of habits and provide novel insights into potential pharmacological strategies for reducing habitual behaviors in mental disorders. [ABSTRACT FROM AUTHOR]

Published
2019
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33. Neurochemical and Behavioral Dissections of Decision-Making in a Rodent Multistage Task.

Author

Groman, Stephanie M., Mathias, Samuel R., Curry, Daniel W., Lee, Daeyeol, Taylor, Jane R., and Massi, Bart

Abstract

Flexible decision-making in dynamic environments requires both retrospective appraisal of reinforced actions and prospective reasoning about the consequences of actions. These complementary reinforcement-learning systems can be characterized computationally with model-free and model-based algorithms, but how these processes interact at a neurobehavioral level in normal and pathological states is unknown. Here, we developed a translationally analogous multistage decision-making (MSDM) task to independently quantify modelfree and model-based behavioral mechanisms in rats. We provide the first direct evidence that male rats, similar to humans, use both model-free and model-based learning when making value-based choices in the MSDM task and provide novel analytic approaches for independently quantifying these reinforcement-learning strategies. Furthermore, we report that ex vivo dopamine tone in the ventral striatum and orbitofrontal cortex correlate with model-based, but not model-free, strategies, indicating that the biological mechanisms mediating decision-making in the multistage task are conserved in rats and humans. This new multistage task provides a unique behavioral platform for conducting systems-level analyses of decision-making in normal and pathological states. [ABSTRACT FROM AUTHOR]

Published
2019
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34. Dissecting Impulsivity and its Relationships to Drug Addictions

Author

Jentsch, J. David, Ashenhurst, James R., Cervantes, M. Catalina, James, Alexander S., Groman, Stephanie M., and Pennington, Zachary T.

Subjects
Neurons, Receptors, Dopamine D2, Substance-Related Disorders, Brain, Down-Regulation, Nerve Tissue Proteins, Synaptic Transmission, Article, Behavior, Addictive, Translational Research, Biomedical, Risk Factors, Impulsive Behavior, Animals, Humans, Disease Susceptibility, Serotonergic Neurons
Abstract

Addictions are often characterized as forms of impulsive behavior. That said, it is often noted that impulsivity is a multidimensional construct, spanning several psychological domains. This review describes the relationship between varieties of impulsivity and addiction-related behaviors, the nature of the causal relationship between the two and the underlying neurobiological mechanisms that promote impulsive behaviors. We conclude that the available data strongly supports the notion that impulsivity is both a risk factor for, and a consequence of, drug and alcohol consumption. While the evidence indicating that subtypes of impulsive behavior are uniquely informative – either biologically or with respect to their relationships to addictions – is convincing, multiple lines of study link “distinct” subtypes of impulsivity to low dopamine D2 receptor function and perturbed serotonergic transmission, revealing shared mechanisms between the subtypes. Therefore, a common biological framework involving monoaminergic transmitters in key frontostriatal circuits may link multiple forms of impulsivity to drug self-administration and addiction-related behaviors. Further dissection of these relationships is needed before the next phase of genetic and genomic discovery will be able to reveal the biological sources of the vulnerability for addiction indexed by impulsivity.

Published
2014

35. Dopamine D3 Receptor Availability Is Associated with Inflexible Decision Making.

Author

Groman, Stephanie M., Smith, Nathaniel J., Petrullli, J. Ryan, Massi, Bart, Lihui Chen, Ropchan, Jim, Yiyun Huang, Daeyeol Lee, Morris, Evan D., and Taylor, Jane R.

Subjects
*DOPAMINE receptors, *BRAIN imaging, *INDIVIDUAL differences, *DECISION making, *RADIOLIGAND assay, *REINFORCEMENT learning, *COMPUTATIONAL neuroscience
Abstract

Dopamine D2/3 receptor signaling is critical for flexible adaptive behavior; however, it is unclear whether D2, D3, or both receptor subtypes modulate precise signals of feedback and reward history that underlie optimal decision making. Here, PET with the radioligand [11C]-(+)-PHNO was used to quantify individual differences in putative D3 receptor availability in rodents trained on a novel threechoice spatial acquisition and reversal-learning task with probabilistic reinforcement. Binding of [11C)-(+)-PHNO in the midbrain was negatively related to the ability of rats to adapt to changes in rewarded locations, but not to the initial learning. Computational modeling of choice behavior in the reversal phase indicated that [11C]-(+)-PHNO binding in the midbrain was related to the learning rate and sensitivity to positive, but not negative, feedback. Administration of a D3-preferring agonist likewise impaired reversal performance by reducing the learning rate and sensitivity to positive feedback. These results demonstrate a previously unrecognized role for D3 receptors in select aspects of reinforcement learning and suggest that individual variation in midbrain D3 receptors influences flexible behavior. Our combined neuroimaging, behavioral, pharmacological, and computational approach implicates the dopamine D3 receptor in decision-making processes that are altered in psychiatric disorders. [ABSTRACT FROM AUTHOR]

Published
2016
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36. Primate Phencyclidine Model of Schizophrenia: Sex-Specific Effects on Cognition, Brain Derived Neurotrophic Factor, Spine Synapses, and Dopamine Turnover in Prefrontal Cortex.

Author

Elsworth, John D., Groman, Stephanie M., Jentsch, James D., Leranth, Csaba, Redmond Jr, D. Eugene, Kim, Jung D., Diano, Sabrina, and Roth, Robert H.

Subjects
SCHIZOPHRENIA treatment, PHENCYCLIDINE, COGNITION, NEUROTROPHINS, SYNAPSES, PHYSIOLOGICAL effects of dopamine, PREFRONTAL cortex
Abstract

Background: Cognitive deficits are a core symptom of schizophrenia, yet they remain particularly resistant to treatment. The model provided by repeatedly exposing adult nonhuman primates to phencyclidine has generated important insights into the neurobiology of these deficits, but it remains possible that administration of this psychotomimetic agent during the pre-adult period, when the dorsolateral prefrontal cortex in human and nonhuman primates is still undergoing significant maturation, may provide a greater understanding of schizophrenia-related cognitive deficits. Methods: The effects of repeated phencyclidine treatment on spine synapse number, dopamine turnover and BDNF expression in dorsolateral prefrontal cortex, and working memory accuracy were examined in pre-adult monkeys. Results: One week following phencyclidine treatment, juvenile and adolescent male monkeys demonstrated a greater loss of spine synapses in dorsolateral prefrontal cortex than adult male monkeys. Further studies indicated that in juvenile males, a cognitive deficit existed at 4 weeks following phencyclidine treatment, and this impairment was associated with decreased dopamine turnover, decreased brain derived neurotrophic factor messenger RNA, and a loss of dendritic spine synapses in dorsolateral prefrontal cortex. In contrast, female juvenile monkeys displayed no cognitive deficit at 4 weeks after phencyclidine treatment and no alteration in dopamine turnover or brain derived neurotrophic factor messenger RNA or spine synapse number in dorsolateral prefrontal cortex. In the combined group of male and female juvenile monkeys, significant linear correlations were detected between dopamine turnover, spine synapse number, and cognitive performance. Conclusions: As the incidence of schizophrenia is greater in males than females, these findings support the validity of the juvenile primate phencyclidine model and highlight its potential usefulness in understanding the deficits in dorsolateral prefrontal cortex in schizophrenia and developing novel treatments for the cognitive deficits associated with schizophrenia. [ABSTRACT FROM AUTHOR]

Published
2015
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37. In the Blink of an Eye: Relating Positive-Feedback Sensitivity to Striatal Dopamine D2-Like Receptors through Blink Rate.

Author

Groman, Stephanie M., James, Alex S., Seu, Emanuele, Tran, Steven, Clark, Taylor A., Harpster, Sandra N., Crawford, Maverick, Burtner, Joanna Lee, Feiler, Karen, Roth, Robert H., Elsworth, John D., London, Edythe D., and Jentsch, James David

Subjects
*BLINKING (Physiology), *DOPAMINERGIC mechanisms, *POSITRON emission tomography, *BIOMARKERS, *DOPAMINE receptors, *CERCOPITHECUS aethiops
Abstract

For >30 years, positron emission tomography (PET) has proven to be a powerful approach for measuring aspects of dopaminergic transmission in the living human brain; this technique has revealed important relationships between dopamine D2-like receptors and dimensions of normal behavior, such as human impulsivity, and psychopathology, particularly behavioral addictions. Nevertheless, PET is an indirect estimate that lacks cellular and functional resolution and, in some cases, is not entirely pharmacologically specific. To identify the relationships between PET estimates of D2-like receptor availability and direct in vitro measures of receptor number, affinity, and function, we conducted neuroimaging and behavioral and molecular pharmacological assessments in a group of adult male vervet monkeys. Data gathered from these studies indicate that variation in D2-like receptor PET measurements is related to reversal-learning performance and sensitivity to positive feedback and is associated with in vitro estimates of the density of functional dopamine D2-like receptors. Furthermore, we report that a simple behavioral measure, eyeblink rate, reveals novel and crucial links between neuroimaging assessments and in vitro measures of dopamine D2 receptors. [ABSTRACT FROM AUTHOR]

Published
2014
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38. An Evaluation of the Evidence that Methamphetamine Abuse Causes Cognitive Decline in Humans.

Author

Dean, Andy C, Groman, Stephanie M, Morales, Angelica M, and London, Edythe D

Subjects
*METHAMPHETAMINE abuse, *COGNITION, *ADULTS, *TEMPERANCE, *CROSS-sectional method
Abstract

Methamphetamine (MA) is one of the most commonly abused illicit substances worldwide. Among other problems, abuse of the drug has been associated with reduced cognitive function across several domains. However, much of the literature has not attempted to differentiate cognitive difficulties caused by MA abuse from preexisting cognitive difficulties that are likely caused by other factors. Here, we address this question, evaluating evidence for a priori hypotheses pertaining to six lines of research: (a) animal studies; (b) cross-sectional human studies; (c) a twin study; (d) studies of changes in cognition with abstinence from MA; (e) studies of changes in brain structure and function with abstinence from MA; and (f) studies of the relationship between the severity of MA abuse and the extent of cognitive deficits observed. Overall the findings were mixed, with some support for a causal relationship between MA abuse and cognitive decline, and other findings suggesting that there is no relationship. The preponderance of the data, however, does support the possibility that MA abuse causes cognitive decline, of unknown duration, in at least some users of the drug. When averaged across individuals, this decline is likely to be mild in early-to-middle adulthood. However, moderator variables are likely to contribute to the presence and/or severity of cognitive decline exhibited by a given individual. [ABSTRACT FROM AUTHOR]

Published
2013
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39. Dysregulation of D2-Mediated Dopamine Transmission in Monkeys after Chronic Escalating Methamphetamine Exposure.

Author

Groman, Stephanie M., Lee, Buyean, Seu, Emanuele, James, Alex S., Feiler, Karen, Mandelkern, Mark A., London, Edythe D., and Jentsch, J. David

Subjects
*DOPAMINE regulation, *LABORATORY monkeys, *NEURAL transmission, *METHAMPHETAMINE, *SUBSTANCE abuse, *DOPAMINERGIC neurons, *NEUROCHEMISTRY
Abstract

Compulsive drug-seeking and drug-taking are important substance-abuse behaviors that have been linked to alterations in dopaminergic neurotransmission and to impaired inhibitory control. Evidence supports the notions that abnormal D2 receptor-mediated dopamine transmission and inhibitory control may be heritable risk factors for addictions, and that they also reflect drug-induced neuroadaptations. To provide a mechanistic explanation for the drug-induced emergence of inhibitory-control deficits, this study examined how a chronic, escalating-dose regimen of methamphetamine administration affected dopaminergic neurochemistry and cognition in monkeys. DopamineD2-like receptor and dopamine transporter (DAT) availability and reversal-learning performance were measured before and after exposure to methamphetamine (or saline), and brain dopamine levels were assayed at the conclusion of the study. Exposure to methamphetamine reduced dopamine D2-like receptor and DAT availability and produced transient, selective impairments in the reversal of a stimulus- outcome association. Furthermore, individual differences in the change in D2-like receptor availability in the striatum were related to the change in response to positive feedback. These data provide evidence that chronic, escalating-dose methamphetamine administration alters the dopamine system in a manner similar to that observed in methamphetamine-dependent humans. They also implicate alterations in positive-feedback sensitivity associated with D2-like receptor dysfunction as the mechanism by which inhibitory control deficits emerge in stimulant-dependent individuals. Finally, a significant degree of neurochemical and behavioral variation in response to methamphetamine was detected, indicating that individual differences affect the degree to which drugs of abuse alter these processes. Identification of these factors ultimately may assist in the development of individualized treatments for substance dependence. [ABSTRACT FROM AUTHOR]

Published
2012
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40. Cognitive control and the dopamine D2-like receptor: a dimensional understanding of addiction.

Author

Groman, Stephanie M. and Jentsch, J. David

Subjects
*DOPAMINE receptors, *ADDICTIONS, *COGNITIVE ability, *HETEROGENEITY, *MENTAL depression, *ANXIETY disorders, *TREATMENT effectiveness
Abstract

The phenotypic complexity of psychiatric conditions is revealed by the dimensional nature of these disorders, which consist of multiple behavioral, affective, and cognitive dysfunctions that can result in substantial psychosocial impairment. The high degree of heterogeneity in symptomatology and comorbidity suggests that simple categorical diagnoses of 'affected' or 'unaffected' may fail to capture the true characteristics of the disorder in a manner relevant to individualized treatment. A particular dimension of interest is cognitive control ability because impairments in the capacity to control thoughts, feelings, and actions are key to several psychiatric disorders. Here, we describe evidence suggesting that cognitive control over behavior is a crucial dimension of function relevant to addictions. Moreover, dopamine (DA) D2-receptor transmission is increasingly being identified as a point of convergence for these behavioral and cognitive processes. Consequently, we argue that measures of cognitive control and D2 DA receptor function may be particularly informative markers of individual function and treatment response in addictions. Depression and Anxiety 0:1-12, 2011. © 2011 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published
2012
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41. Dorsal Striatal D2-Like Receptor Availability Covaries with Sensitivity to Positive Reinforcement during Discrimination Learning.

Author

Groman, Stephanie M., Lee, Buyean, London, Edythe D., Mandelkern, Mark A., James, Alex S., Feiler, Karen, Rivera, Ronald, Dahlbom, Magnus, Sossi, Vesna, Vandervoort, Eric, and Jentsch, J. David

Subjects
*DOPAMINE, *DISCRIMINATION learning, *BRAIN imaging, *POSITRON emission tomography, *NEUROBEHAVIORAL disorders
Abstract

Deviations in reward sensitivity and behavioral flexibility, particularly in the ability to change or stop behaviors in response to changing environmental contingencies, are important phenotypic dimensions of several neuropsychiatric disorders. Neuroimaging evidence suggests that variation in dopamine signaling through dopamine D2-like receptors may influence these phenotypes, as well as associated psychiatric conditions, but the specific neurocognitive mechanisms through which this influence is exerted are unknown. To address this question, we examined the relationship between behavioral sensitivity to reinforcement during discrimination learning and D2-like receptor availability in vervet monkeys. Monkeys were assessed for their ability to acquire, retain, and reverse three-choice, visual discrimination problems, and once behavioral performance had stabilized, they received positron emission tomography (PET) scans. D2-like receptor availability in dorsal aspects of the striatum was not related to individual differences in the ability to acquire or retain visual discriminations but did relate to the number of trials required to reach criterion in the reversal phase of the task. D2-like receptor availability was also strongly correlated with behavioral sensitivity to positive, but not negative, feedback during learning. These results go beyond electrophysiological findings by demonstrating the involvement of a striatal dopaminergic marker in individual differences in feedback sensitivity and behavioral flexibility, providing insight into the neural mechanisms that are affected in neuropsychiatric disorders that feature these deficits. [ABSTRACT FROM AUTHOR]

Published
2011
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42. Behavioral Characteristics and Neural Mechanisms Mediating Performance in a Rodent Version of the Balloon Analog Risk Task.

Author

Jentsch, James David, Woods, Jason A., Groman, Stephanie M., and Seu, Emanuele

Subjects
RISK-taking behavior, BEHAVIOR, SUBSTANCE abuse, GAMBLING, CEREBRAL cortex, PUBLIC health
Abstract

The tendency for some individuals to partake in high-risk behaviors (eg, substance abuse, gambling, risky sexual activities) is a matter of great public health concern, yet the characteristics and neural bases of this vulnerability are largely unknown. Recent work shows that this susceptibility can be partially predicted by laboratory measures of reward seeking under risk, including the Balloon Analog Risk Task. Rats were trained to respond on two levers: one of which (the ‘add lever’) increased the size of a potential food reward and a second (the ‘cash-out lever’) that led to delivery of accrued reward. Crucially, each add-lever response was also associated with a risk that the trial would fail and no reward would be delivered. The relative probabilities that each add-lever press would lead to an addition food pellet or to trial failure (risk) were orthogonally varied. Rats exhibited a pattern of responding characteristic of incentive motivation and risk aversion, with a subset of rats showing traits of high-risk taking and/or suboptimal responding. Neural inactivation studies suggest that the orbitofrontal cortex supports greater reward seeking in the presence or absence of risk, whereas the medial prefrontal cortex is required for optimization of patterns of responding. These findings provide new information about the neural circuitry of decision making under risk and reveal new insights into the biological determinants of risk-taking behaviors that may be useful in developing biomarkers of vulnerability. [ABSTRACT FROM AUTHOR]

Published
2010
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43. Dimensions of Impulsivity Are Associated with Poor Spatial Working Memory Performance in Monkeys.

Author

James, Alex S., Groman, Stephanie M., Seu, Emanuele, Jorgensen, Matthew, Fairbanks, Lynn A., and Jentsch, J. David

Subjects
*SHORT-term memory, *MONKEYS, *DOPAMINE, *ATTENTION-deficit hyperactivity disorder, *COGNITION, *TEMPERAMENT, *SEROTONIN, *PREFRONTAL cortex
Abstract

Impulsive behavior and novelty seeking are dimensions of temperament that are behavioral determinants of risk for attention deficit/ hyperactivity disorder and its neurocognitive endophenotypes, and variation in the dopamine D4 receptor gene (DRD4) explains at least a portion of the variance in the traits. To further characterize the dimensional phenotype associated with impulsiveness, adolescent male monkeys were evaluated using ecologically valid tests of impulsive approach and aggression in response to social or nonsocial stimuli; subsequently, a delayed response task was implemented to assess spatial working memory performance. Subjects were selected into this study based on their response to the social challenge task or by DRD4 genotype, resulting in three groups: low-impulsivity/common DRD4 allele, high-impulsivity/common DRD4 allele, or rare DRD4 allele. All animals acquired the delayed response task and could perform at near ceiling levels when a ~0 s delay version was imposed, but as delays were lengthened, high-impulsive animals, regardless of DRD4 genotype, made fewer correct responses than did low-impulsive subjects; an inverse relationship existed for working memory and impulsivity. Notably, impulsive behavior evoked by social and nonsocial stimuli explained overlapping and independent portions of the variance in working memory performance. CSF levels of monoamine metabolites did not significantly differentiate the high- and low-impulsive animals, although monkeys carrying the DRD4 rare allele tended to exhibit higher monoamine turnover. These data indicate that dimensions of impulsivity may impact on working memory performance in qualitatively similar ways but through different mechanisms. [ABSTRACT FROM AUTHOR]

Published
2007
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45. Sex differences in oxycodone-taking behaviors are linked to disruptions in reward-guided, decision-making functions.

Author

LaRocco K, Villiamma P, Hill J, Russell MA, DiLeone RJ, and Groman SM

Abstract

Problematic opioid use that emerges in a subset of individuals may be due to pre-existing disruptions in the biobehavioral mechanisms that regulate drug use. The identity of these mechanisms is not known, but emerging evidence suggests that suboptimal decision-making that is observable prior to drug use may contribute to the pathology of addiction and, notably, serve as a powerful phenotype for interrogating biologically based differences in opiate-taking behaviors. The current study investigated the relationship between decision-making phenotypes and opioid-taking behaviors in male and female Long Evans rats. Adaptive decision-making processes were assessed using a probabilistic reversal-learning task and oxycodone- (or vehicle, as a control) taking behaviors assessed for 32 days using a saccharin fading procedure that promoted dynamic intake of oxycodone. Tests of motivation, extinction, and reinstatement were also performed. Computational analyses of decision-making and opioid-taking behaviors revealed that attenuated reward-guided decision-making was associated with greater self-administration of oxycodone and addiction-relevant behaviors. Moreover, pre-existing impairments in reward-guided decision-making observed in female rats was associated with greater oxycodone use and addiction-relevant behaviors when compared to males. These results provide new insights into the biobehavioral mechanisms that regulate opiate-taking behaviors and offer a novel phenotypic approach for interrogating sex differences in addiction susceptibility and opioid use disorders.

Published
2024
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46. Reward-Mediated, Model-Free Reinforcement-Learning Mechanisms in Pavlovian and Instrumental Tasks Are Related.

Author

Moin Afshar N, Cinotti F, Martin D, Khamassi M, Calu DJ, Taylor JR, and Groman SM

Subjects
Rats, Male, Animals, Learning, Motivation, Conditioning, Operant, Cues, Reinforcement, Psychology, Reward
Abstract

Model-free and model-based computations are argued to distinctly update action values that guide decision-making processes. It is not known, however, if these model-free and model-based reinforcement learning mechanisms recruited in operationally based instrumental tasks parallel those engaged by pavlovian-based behavioral procedures. Recently, computational work has suggested that individual differences in the attribution of incentive salience to reward predictive cues, that is, sign- and goal-tracking behaviors, are also governed by variations in model-free and model-based value representations that guide behavior. Moreover, it is not appreciated if these systems that are characterized computationally using model-free and model-based algorithms are conserved across tasks for individual animals. In the current study, we used a within-subject design to assess sign-tracking and goal-tracking behaviors using a pavlovian conditioned approach task and then characterized behavior using an instrumental multistage decision-making (MSDM) task in male rats. We hypothesized that both pavlovian and instrumental learning processes may be driven by common reinforcement-learning mechanisms. Our data confirm that sign-tracking behavior was associated with greater reward-mediated, model-free reinforcement learning and that it was also linked to model-free reinforcement learning in the MSDM task. Computational analyses revealed that pavlovian model-free updating was correlated with model-free reinforcement learning in the MSDM task. These data provide key insights into the computational mechanisms mediating associative learning that could have important implications for normal and abnormal states. SIGNIFICANCE STATEMENT Model-free and model-based computations that guide instrumental decision-making processes may also be recruited in pavlovian-based behavioral procedures. Here, we used a within-subject design to test the hypothesis that both pavlovian and instrumental learning processes were driven by common reinforcement-learning mechanisms. Sign-tracking and goal-tracking behaviors were assessed in rats using a pavlovian conditioned approach task, and then instrumental behavior was characterized using an MSDM task. We report that sign-tracking behavior was associated with greater model-free, but not model-based, learning in the MSDM task. These data suggest that pavlovian and instrumental behaviors may be driven by conserved reinforcement-learning mechanisms., (Copyright © 2023 the authors.)

Published
2023
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47. Paranoia and belief updating during a crisis.

Author

Suthaharan P, Reed EJ, Leptourgos P, Kenney J, Uddenberg S, Mathys CD, Litman L, Robinson J, Moss AJ, Taylor JR, Groman SM, and Corlett PR

Abstract

The 2019 coronavirus (COVID-19) pandemic has made the world seem unpredictable. During such crises we can experience concerns that others might be against us, culminating perhaps in paranoid conspiracy theories. Here, we investigate paranoia and belief updating in an online sample (N=1,010) in the United States of America (U.S.A). We demonstrate the pandemic increased individuals' self-rated paranoia and rendered their task-based belief updating more erratic. Local lockdown and reopening policies, as well as culture more broadly, markedly influenced participants' belief-updating: an early and sustained lockdown rendered people's belief updating less capricious. Masks are clearly an effective public health measure against COVID-19. However, state-mandated mask wearing increased paranoia and induced more erratic behaviour. Remarkably, this was most evident in those states where adherence to mask wearing rules was poor but where rule following is typically more common. This paranoia may explain the lack of compliance with this simple and effective countermeasure. Computational analyses of participant behaviour suggested that people with higher paranoia expected the task to be more unstable, but at the same time predicted more rewards. In a follow-up study we found people who were more paranoid endorsed conspiracies about mask-wearing and potential vaccines - again, mask attitude and conspiratorial beliefs were associated with erratic task behaviour and changed priors. Future public health responses to the pandemic might leverage these observations, mollifying paranoia and increasing adherence by tempering people's expectations of other's behaviour, and the environment more broadly, and reinforcing compliance.

Published
2021
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48. Reinforcement Learning during Adolescence in Rats.

Author

Moin Afshar N, Keip AJ, Taylor JR, Lee D, and Groman SM

Subjects
Age Factors, Animals, Female, Humans, Male, Rats, Rats, Long-Evans, Conditioning, Operant physiology, Reinforcement, Psychology, Reversal Learning physiology
Abstract

The most dynamic period of postnatal brain development occurs during adolescence, the period between childhood and adulthood. Neuroimaging studies have observed morphologic and functional changes during adolescence, and it is believed that these changes serve to improve the functions of circuits that underlie decision-making. Direct evidence in support of this hypothesis, however, has been limited because most preclinical decision-making paradigms are not readily translated to humans. Here, we developed a reversal-learning protocol for the rapid assessment of adaptive choice behavior in dynamic environments in rats as young as postnatal day 30. A computational framework was used to elucidate the reinforcement-learning mechanisms that change in adolescence and into adulthood. Using a cross-sectional and longitudinal design, we provide the first evidence that value-based choice behavior in a reversal-learning task improves during adolescence in male and female Long-Evans rats and demonstrate that the increase in reversal performance is due to alterations in value updating for positive outcomes. Furthermore, we report that reversal-learning trajectories in adolescence reliably predicted reversal performance in adulthood. This novel behavioral protocol provides a unique platform for conducting biological and systems-level analyses of the neurodevelopmental mechanisms of decision-making. SIGNIFICANCE STATEMENT The neurodevelopmental adaptations that occur during adolescence are hypothesized to underlie age-related improvements in decision-making, but evidence to support this hypothesis has been limited. Here, we describe a novel behavioral protocol for rapidly assessing adaptive choice behavior in adolescent rats with a reversal-learning paradigm. Using a computational approach, we demonstrate that age-related changes in reversal-learning performance in male and female Long-Evans rats are linked to specific reinforcement-learning mechanisms and are predictive of reversal-learning performance in adulthood. Our behavioral protocol provides a unique platform for elucidating key components of adolescent brain function., (Copyright © 2020 the authors.)

Published
2020
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49. The Neurobiology of Impulsive Decision-Making and Reinforcement Learning in Nonhuman Animals.

Author

Groman SM

Subjects
Animals, Choice Behavior, Decision Making, Dopamine, Humans, Neurobiology, Reward, Impulsive Behavior, Reinforcement, Psychology
Abstract

Impulsive decisions are those that favor immediate over delayed rewards, involve the acceptance of undue risk or uncertainty, or fail to adapt to environmental changes. Pathological levels of impulsive decision-making have been observed in individuals with mental illness, but there may be substantial heterogeneity in the processes that drive impulsive choices. Understanding this behavioral heterogeneity may be critical for understanding associated diverseness in the neural mechanisms that give rise to impulsivity. The application of reinforcement learning algorithms in the deconstruction of impulsive decision-making phenotypes can help bridge the gap between biology and behavior and provide insights into the biobehavioral heterogeneity of impulsive choice. This chapter will review the literature on the neurobiological mechanisms of impulsive decision-making in nonhuman animals; specifically, the role of the amine neuromodulatory systems (dopamine, serotonin, norepinephrine, and acetylcholine) in impulsive decision-making and reinforcement learning processes is discussed. Ultimately, the integration of reinforcement learning algorithms with sophisticated behavioral and neuroscience techniques may be critical for advancing the understanding of the neurochemical basis of impulsive decision-making.

Published
2020
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50. Chronic Exposure to Methamphetamine Disrupts Reinforcement-Based Decision Making in Rats.

Author

Groman SM, Rich KM, Smith NJ, Lee D, and Taylor JR

Subjects
Animals, Benzazepines administration & dosage, Decision Making physiology, Male, Rats, Rats, Long-Evans, Central Nervous System Stimulants administration & dosage, Central Nervous System Stimulants adverse effects, Decision Making drug effects, Methamphetamine administration & dosage, Methamphetamine adverse effects, Reinforcement, Psychology
Abstract

The persistent use of psychostimulant drugs, despite the detrimental outcomes associated with continued drug use, may be because of disruptions in reinforcement-learning processes that enable behavior to remain flexible and goal directed in dynamic environments. To identify the reinforcement-learning processes that are affected by chronic exposure to the psychostimulant methamphetamine (MA), the current study sought to use computational and biochemical analyses to characterize decision-making processes, assessed by probabilistic reversal learning, in rats before and after they were exposed to an escalating dose regimen of MA (or saline control). The ability of rats to use flexible and adaptive decision-making strategies following changes in stimulus-reward contingencies was significantly impaired following exposure to MA. Computational analyses of parameters that track choice and outcome behavior indicated that exposure to MA significantly impaired the ability of rats to use negative outcomes effectively. These MA-induced changes in decision making were similar to those observed in rats following administration of a dopamine D2/3 receptor antagonist. These data use computational models to provide insight into drug-induced maladaptive decision making that may ultimately identify novel targets for the treatment of psychostimulant addiction. We suggest that the disruption in utilization of negative outcomes to adaptively guide dynamic decision making is a new behavioral mechanism by which MA rigidly biases choice behavior.

Published
2018
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