Your search keyword '"Drug addiction"' showing total 414 results

1. The mGlu5 receptor negative allosteric modulator mavoglurant reduces escalated cocaine self-administration in male and female rats.

Author

Vendruscolo, Leandro F., Vendruscolo, Janaina C.M., Whiting, Kimberly E., Acri, Jane B., Volkow, Nora D., and Koob, George F.

Subjects

*COCAINE-induced disorders, *COCAINE abuse, *ORAL drug administration, *DRUG therapy, *LABORATORY rats

Abstract

Rationale: Cocaine use disorder (CUD) is a brain disorder for which there is no Food and Drug Administration-approved pharmacological treatment. Evidence suggests that glutamate and metabotropic glutamate receptor subtype 5 (mGlu5) play critical roles in synaptic plasticity, neuronal development, and psychiatric disorders. Objective: In the present study, we tested the hypothesis that the mGlu5 receptor is functionally involved in intravenous cocaine self-administration and assessed the effects of sex and cocaine exposure history. Methods: We used a preclinical model of CUD in rats that were allowed long access (LgA; 6 h/day) or short access (ShA; 1 h/day) to intravenous cocaine (750 µg/kg/infusion [0.1 ml]) self-administration. Rats received acute intraperitoneal or oral administration of the mGlu5 receptor negative allosteric modulator mavoglurant (1, 3, and 10 mg/kg) or vehicle. Results: Both intraperitoneal and oral mavoglurant administration dose-dependently reduced intravenous cocaine self-administration in the first hour and in the entire 6 h session in rats in the LgA group, with no effect on locomotion. In the ShA group, mavoglurant decreased locomotion but had no effects on cocaine self-administration. We did not observe significant sex × treatment interactions. Conclusions: These findings suggest that the mGlu5 receptor is involved in escalated cocaine self-administration. These findings support the development of clinical trials of mavoglurant to evaluate its potential therapeutic benefits for CUD. [ABSTRACT FROM AUTHOR]

Published

2024

2. The secondary visual cortex mediated the enhancement of associative learning on methamphetamine self-administration behaviors.

Author

Wang, Cai-ling, Cao, Dan-ni, Wu, Ning, Zhu, Ying-jie, and Li, Jin

Subjects

*ASSOCIATIVE learning, *VISUAL cortex, *DRUG addiction, *METHAMPHETAMINE, *SUCROSE

Abstract

Rationale: Methamphetamine addiction is a persistent and intractable pathological learning and memory, whereas no approved therapeutics is available. However, few attentions have been paid to how associative learning participates in the formation of intractable memory related to drug addiction Objectives and methods: To investigate the role of associative learning in methamphetamine addiction and the underlying neurobiological mechanism, methamphetamine self-administration, oral sucrose self-administration, chemogenetic neuromanipulation, and fiber photometry in mice were performed in this study. Results: We reported that associative learning increased methamphetamine-induced self-administration, but not oral sucrose self-administration. In addition, the enhancement of methamphetamine-induced self-administration was independent of more methamphetamine consumption, and remained with higher drug-taking and motivation in the absence of visual cues, suggesting the direct effects of the associative learning that enhanced methamphetamine-induced self-administration. Moreover, chemogenetic inactivation of the secondary visual cortex (V2) reduced the enhancement of the drug-taking induced by associative learning but did not alter sucrose-taking. Further fiber photometry of V2 neurons demonstrated that methamphetamine-associative learning elicits V2 neuron excitation, and sucrose-associative learning elicits V2 neuron inhibition. Conclusions: Therefore, this study reveals the neurobiological mechanism of V2 excitability underlying how associative learning participates in the formation of intractable memory related to drug addiction, and gives evidence to support V2 as a promising target for stimulation therapy for methamphetamine addiction. [ABSTRACT FROM AUTHOR]

Published

2024

3. METH exposure alters sperm DNA methylation in F0 mice and mPFC transcriptome in male F1 mice.

Author

Li, Zhaosu, Liu, Dekang, Wang, Guanxiong, Zheng, Yanyan, Chen, Liying, Cheng, Zhen, Zhang, Zijing, Cai, Qinglong, Ge, Feifei, Fan, Yu, and Guan, Xiaowei

Subjects

*METHAMPHETAMINE, *DNA methylation, *TRANSCRIPTOMES, *SPERMATOZOA, *DRUG addiction, *PREFRONTAL cortex, *NEURAL development

Abstract

Rationale: Methamphetamine (METH) exposure has toxicity in sperm epigenetic phenotype and increases the risk for developing addiction in their offspring. However, the underlying transgenerational mechanism remains unclear. Objectives: The current study aims to investigate the profiles of sperm epigenetic modifications in male METH-exposed mice (F0) and medial prefrontal cortex (mPFC) transcriptome in their male first-generation offspring (F1). Methods: METH-related male F0 and F1 mice model was established to investigate the effects of paternal METH exposure on reproductive functions and sperm DNA methylation in F0 and mPFC transcriptomic profile in F1. During adulthood, F1 was subjected to a conditioned place preference (CPP) test to evaluate sensitivity to METH. The gene levels were verified with qPCR. Results: METH exposure obviously altered F0 sperms DNA methylated profile and male F1 mPFC transcriptomic profile, many of which being related to neuronal system and brain development. In METH-sired male F1, subthreshold dose of METH administration effectively elicited CPP, along with more mPFC activation. After qPCR verification, Sort1 and Shank2 were at higher levels in F0 sperm and F1 mPFC. Conclusions: Our findings put new insights into paternal METH exposure-altered profiles of F0 sperm DNA methylation and male F1 mPFC transcriptomics. Several genes, such as Sort1 and Shank2, might be used as potential molecules for further research on the transgenerational vulnerability to drug addiction in offspring by paternal drug exposure. [ABSTRACT FROM AUTHOR]

Published

2024

4. Individual differences in GHB consumption in a new voluntary GHB self-administration model in outbred rats.

Author

Wolf, Casper J. H., Spoelder, Marcia, Beurmanjer, Harmen, Bulthuis, Ronald, Schellekens, Arnt F. A., and Homberg, Judith R.

Subjects

*OPERANT behavior, *RATS, *INDIVIDUAL differences, *DRUG abuse, *LONG-term memory, *DRUG withdrawal symptoms, *MAZE tests

Abstract

Background and purpose: The use of the recreational drug gamma-hydroxybutyric acid (GHB) has increased over the past decade, concomitantly leading to a higher incidence of GHB use disorder. Evidence-based treatment interventions are hardly available and cognitive effects of long-term GHB use remain elusive. In order to study the development of GUD and the causal effects of chronic GHB consumption, a GHB self-administration model is required. Experimental approach: Long Evans rats had access to GHB in their home cage according to a two-bottle choice procedure for 3 months. Intoxication and withdrawal symptoms were assessed using an automated sensor-based setup for longitudinal behavioral monitoring. Rats were trained in an operant environment according to a fixed ratio (FR) 1, 2, and 4 schedule of reinforcement. Addiction-like behaviors were assessed through progressive ratio-, non-reinforced-, and quinine-adulterated operant tests. In addition, the novel object recognition test and elevated plus maze test were performed before and after GHB self-administration to assess memory performance and anxiety-like behavior, respectively. Key results: All rats consumed pharmacologically relevant levels of GHB in their home cage, and their intake remained stable over a period of 3 months. No clear withdrawal symptoms were observed following abstinence. Responding under operant conditions was characterized by strong inter-individual differences, where only a subset of rats showed high motivation for GHB, habitual GHB-seeking, and/or continued responding for GHB despite an aversive taste. Male rats showed a reduction in long-term memory performance 3 months after home-cage GHB self-administration. Anxiety-like behavior was not affected by GHB self-administration. Conclusion and implications: The GHB self-administration model was able to reflect individual susceptibility for addiction-like behavior. The reduction in long-term memory performance upon GHB self-administration calls for further research into the cognitive effects of chronic GHB use in humans. [ABSTRACT FROM AUTHOR]

Published

2024

5. An economon model of drug addiction.

Author

Negus, S. Stevens

Subjects

*DRUG addiction, *OPERANT behavior, *SUBSTANCE abuse, *SOCIAL networks, *ADDICTIONS

Abstract

The term "economon" (i:'ka.nə.muhn; plural: economa) is introduced here to describe an economic unit composed of two participants engaged in mutually reinforcing operant behavior. Economa are basic building blocks of transactional behavior that aggregate in social networks called economies. In a drug-addiction economon, operant behavior by one participant (the "supplier") provides an addictive drug as a reinforcer to the second participant (a "Person with Substance Use Disorder; PwSUD"). Reciprocal operant behavior by the PwSUD usually provides money as a reinforcer to the supplier. After defining the features of the drug-addiction economon, this article discusses its implications for (1) prevalence and virulence of drug addiction, (2) opportunities for drug-addiction research in general, (3) the "brain-disease model of addiction" in particular, and (4) factors that mitigate harm or promote risk of drug addiction. The economon model is intended to provide a novel perspective on the uniquely human disorder of drug addiction. [ABSTRACT FROM AUTHOR]

Published

2024

6. Novelty-induced locomotor behavior predicts heroin addiction vulnerability in male, but not female, rats.

Author

Kuhn, Brittany N., Cannella, Nazzareno, Crow, Ayteria D., Roberts, Analyse T., Lunerti, Veronica, Allen, Carter, Nall, Rusty W., Hardiman, Gary, Woods, Leah C. Solberg, Chung, Dongjun, Ciccocioppo, Roberto, and Kalivas, Peter W.

Subjects

*HEROIN, *OPIOIDS, *SUBSTANCE-induced disorders, *DRUG addiction, *GENDER differences (Psychology)

Abstract

Rationale: The ongoing rise in opioid use disorder (OUD) has made it imperative to better model the individual variation within the human population that contributes to OUD vulnerability. Using animal models that capture such variation can be a useful tool. Individual variation in novelty-induced locomotion is predictive of substance use disorder (SUD) propensity. In this model, rats are characterized as high-responders (HR) or low-responders (LR) using a median split based on distance travelled during a locomotor test, and HR rats are generally found to exhibit a more SUD vulnerable behavioral phenotype. Objectives: The HR/LR model has commonly been used to assess behaviors in male rats using psychostimulants, with limited knowledge of the predictive efficacy of this model in females or the use of an opioid as the reward. In the current study, we assessed several behaviors across the different phases of drug addiction (heroin taking, refraining, and seeking) in over 500 male and female heterogeneous stock rats run at two geographically separate locations. Rats were characterized as HRs or LRs within each sex for analysis. Results: Overall, females exhibit a more OUD vulnerable phenotype relative to males. Additionally, the HR/LR model was predictive of OUD-like behaviors in male, but not female rats. Furthermore, phenotypes did not differ in anxiety-related behaviors, reacquisition of heroin-taking, or punished heroin-taking behavior in either sex. Conclusions: These results emphasize the importance of assessing females in models of individual variation in SUD and highlight limitations in using the HR/LR model to assess OUD propensity. [ABSTRACT FROM AUTHOR]

Published

2022

7. Characterization of operant social interaction in rats: effects of access duration, effort, peer familiarity, housing conditions, and choice between social interaction vs. food or remifentanil.

Author

Chow, Jonathan J., Beacher, Nicholas J., Chabot, Jules M., Oke, Marvellous, Venniro, Marco, Lin, Da-Ting, and Shaham, Yavin

Subjects

*SOCIAL interaction, *CHOICE (Psychology), *DRUG addiction, *HOUSING, *REMIFENTANIL

Abstract

Rationale and objective: Social factors play a critical role in drug addiction. We recently showed that rats will abstain from methamphetamine, cocaine, heroin, and remifentanil self-administration when given a choice between the addictive drug and operant social interaction. Here, we further characterized operant social interaction by determining the effects of access duration, effort, peer familiarity, and housing conditions. We also determined choice between social interaction vs. palatable food or remifentanil. Methods: We first trained single-housed male and female rats to lever-press for social interaction with a sex- and age-matched peer. Next, we determined effects of access duration (3.75 to 240 s), effort (increasing fixed-ratio schedule requirements or progressive ratio schedule), peer familiarity (familiar vs. unfamiliar), and housing conditions (single vs. paired housing) on social self-administration. We also determined choice between social interaction vs. palatable food pellets or intravenous remifentanil (0, 1, 10 µg/kg/infusion). Results: Increasing access duration to a peer decreased social self-administration under fixed ratio but not progressive ratio schedule; the rats showed similar preference for short vs. long access duration. Social self-administration under different fixed ratio requirements was higher in single-housed than in paired-housed rats and higher for a familiar vs. unfamiliar partner in single-housed but not paired-housed rats. Response rates of food-sated rats under increasing fixed-ratio requirements were higher for palatable food than for social interaction. The rats strongly preferred palatable food over social interaction and showed dose-dependent preference for social interaction vs. remifentanil. Conclusions: We identified parameters influencing the reinforcing effects of operant social interaction and introduce a choice procedure sensitive to remifentanil self-administration dose. [ABSTRACT FROM AUTHOR]

Published

2022

8. The effect of adolescent social isolation on vulnerability for methamphetamine addiction behaviours in female rats.

Author

Webb, Paige I., Hill, Timothy J., Everett, Nicholas A., Thornton, Jade L., Cornish, Jennifer L., and Baracz, Sarah J.

Subjects

*DRUG addiction risk factors, *DRUG addiction, *PSYCHOLOGICAL vulnerability, *ANIMAL experimentation, *MOTIVATION (Psychology), *DISEASE incidence, *METHAMPHETAMINE, *SOCIAL isolation, *RISK assessment, *RATS, *TEENAGERS' conduct of life, *COMPULSIVE behavior, *PSYCHOLOGICAL stress, *ENVIRONMENTAL exposure

Abstract

Rationale: Stress exposure during adolescence contributes to developing a methamphetamine (METH) use disorder. However, most of the studies investigating addiction-related behaviours include only male rodents, despite METH addiction rates being higher in females. Furthermore, animal studies investigating the effects of stress on methamphetamine addiction have used only basic self-administration models which may not be sensitive to the effects of stress. Objectives: This project explored whether adolescent isolation stress exposure increases the incidence of four key addiction-related behaviours in female rats. Methods: Thirty-two female rat pups were caged in groups of four or individually during adolescence from postnatal (PND) day 22, with the latter being re-socialised in groups of four on PND 43. In adulthood, rats were tested for addiction-like behaviours in a METH self-administration paradigm modelling motivation to take METH, persistence in drug-seeking behaviour when METH was not available, resistance to extinction, and propensity to reinstate after a period of withdrawal. Results: Adolescent social isolation resulted in lower METH intake during acquisition; however, the paradigm modelling drug-seeking when the drug was unavailable engendered intermittent METH bingeing in all rats, abolishing the group differences in intake during this phase. Adolescent social isolation also accelerated extinction of non-reinforced lever pressing, and increased stress-primed reinstatement, compared to the group-housed rats. Conclusions: Adolescent social isolation stress alters various methamphetamine addiction-like behaviours in female rats. [ABSTRACT FROM AUTHOR]

Published

2022

9. Investigating individual differences in opioid-taking and opioid-seeking behavior in male rats.

Author

Chang, Stephen E., Krueger, Lauren D., and Flagel, Shelly B.

Subjects

*NARCOTICS, *DRUG addiction, *ANALGESICS, *ANIMAL experimentation, *MOTIVATION (Psychology), *DISEASE relapse, *RATS, *RISK assessment, *SELF medication, *COCAINE, *COMPULSIVE behavior

Abstract

Rationale: Understanding the behavioral and neurobiological factors that render some individuals more susceptible than others to opioid addiction will be critical in combatting the opioid crisis. Objective: The purpose of the current study was to determine if behavioral traits associated with an increased likelihood to take and seek cocaine are the same traits that render one more susceptible to opioid-taking and opioid-seeking behavior. Individual differences in the acquisition of remifentanil self-administration and subsequent cue-induced reinstatement of remifentanil-seeking behavior were investigated using two animal models: the high-responder (HR)/low-responder (LR) and sign-tracker (ST)/goal-tracker (GT) models. Relative to LR rats, HR rats show increased novelty-induced locomotion or "sensation-seeking" behavior, and are more likely to acquire cocaine-taking behavior and do so at a faster rate. Relative to GT rats, ST rats attribute greater incentive motivational value to reward cues and are more likely to exhibit reinstatement of cocaine-seeking behavior. Results: In contrast to previous work using cocaine, we did not observe individual differences with respect to the acquisition of remifentanil self-administration- or cue-induced reinstatement of remifentanil-seeking behavior within the context of either the HR/LR or ST/GT model. Thus, neither the sensation-seeking trait nor the propensity to attribute incentive motivational value to reward cues predicts remifentanil-taking or remifentanil-seeking behavior. Conclusions: These findings suggest that different traits may confer the initiation of opioid- vs. cocaine-taking behavior, and the propensity to relapse to opioid- vs. cocaine-seeking. Additional studies are needed to identify which neurobehavioral constructs confer liability to opioid use and relapse. [ABSTRACT FROM AUTHOR]

Published

2022

10. Inhibition of a cortico-thalamic circuit attenuates cue-induced reinstatement of drug-seeking behavior in "relapse prone" male rats.

Author

Kuhn, Brittany N., Campus, Paolo, Klumpner, Marin S., Chang, Stephen E., Iglesias, Amanda G., and Flagel, Shelly B.

Subjects

*DRUG addiction, *ANIMAL experimentation, *DISEASE relapse, *REINFORCEMENT (Psychology), *THALAMUS, *RATS, *REWARD (Psychology), *COCAINE, *PROMPTS (Psychology), *CEREBRAL cortex, *COMPULSIVE behavior

Abstract

Rationale: Relapse often occurs when individuals are exposed to stimuli or cues previously associated with the drug-taking experience. The ability of drug cues to trigger relapse is believed to be a consequence of incentive salience attribution, a process by which the incentive value of reward is transferred to the reward-paired cue. Sign-tracker (ST) rats that attribute enhanced incentive value to reward cues are more prone to relapse compared to goal-tracker (GT) rats that primarily attribute predictive value to such cues. Objectives: The neurobiological mechanisms underlying this individual variation in relapse propensity remains largely unexplored. The paraventricular nucleus of the thalamus (PVT) has been identified as a critical node in the regulation of cue-elicited behaviors in STs and GTs, including cue-induced reinstatement of drug-seeking behavior. Here we used a chemogenetic approach to assess whether "top-down" cortical input from the prelimbic cortex (PrL) to the PVT plays a role in mediating individual differences in relapse propensity. Results: Chemogenetic inhibition of the PrL-PVT pathway selectively decreased cue-induced reinstatement of drug-seeking behavior in STs, without affecting behavior in GTs. In contrast, cocaine-primed drug-seeking behavior was not affected in either phenotype. Furthermore, when rats were characterized based on a different behavioral phenotype—locomotor response to novelty—inhibition of the PrL-PVT pathway had no effect on either cue- or drug-induced reinstatement. Conclusions: These results highlight an important role for the PrL-PVT pathway in vulnerability to relapse that is consequent to individual differences in the propensity to attribute incentive salience to discrete reward cues. [ABSTRACT FROM AUTHOR]

Published

2022

11. Choosing between cocaine and sucrose under the influence: testing the effect of cocaine tolerance.

Author

Vandaele, Youna and Ahmed, S. H.

Subjects

*DRUG addiction, *DRUG tolerance, *ANIMAL experimentation, *DIETARY sucrose, *TREATMENT effectiveness, *RATS, *COCAINE, *ANOREXIA nervosa, *PHARMACODYNAMICS

Abstract

Rationale: Cocaine use not only depends on the reinforcing properties of the drug, but also on its pharmacological effects on alternative nondrug activities. In animal models investigating choice between cocaine and alternative sweet rewards, the latter influence can have a dramatic impact on choice outcomes. When choosing under cocaine influence is prevented by imposing sufficiently long intervals between choice trials, animals typically prefer the sweet reward. However, when choosing under the drug influence is permitted, animals shift their preference in favor of cocaine. Objectives: We previously hypothesized that this preference shift is mainly due to a direct suppression of responding for sweet reward by cocaine pharmacological effects. Here we tested this hypothesis by making rats tolerant to this drug-induced behavioral suppression. Results: Contrary to our expectation, tolerance did not prevent rats from shifting their preference to cocaine when choosing under the influence. Conclusion: Thus, other mechanisms must be invoked to explain the influence of cocaine intoxication on choice outcomes. [ABSTRACT FROM AUTHOR]

Published

2022

12. "Push it!" or "Hold it!"? A comparison of nicotine-avoidance training and nicotine-inhibition training in smokers motivated to quit.

Author

Machulska, Alla, Rinck, Mike, Klucken, Tim, Kleinke, Kristian, Wunder, Jana-Carina, Remeniuk, Olga, and Margraf, Jürgen

Subjects

*NICOTINE, *SMOKING cessation, *AVOIDANCE conditioning, *NICOTINE addiction, *SMOKING, *CIGARETTE smoke, *DRUG addiction, *COUNSELING, *MOTIVATION (Psychology), *BEHAVIOR, *COMPARATIVE studies, *RANDOMIZED controlled trials, *PRE-tests & post-tests, *STATISTICAL sampling

Abstract

Rationale: Recently, experimental paradigms have been developed to strengthen automatic avoidance or inhibitory responses for smoking cues. However, these procedures have not yet been directly compared regarding their effectiveness and mechanisms of action. Objective: This study compared the effects of avoidance vs. inhibitory training as an add-on to a brief smoking cessation intervention. The standard Approach-Avoidance-Task (AAT) was adapted for both training types and control conditions. Methods: One hundred twenty-four smokers attended behavioral counseling for smoking cessation and were thereafter randomized to one of four training conditions: avoidance-AAT, sham-avoidance-AAT, inhibition-AAT, sham-inhibition-AAT. During a 2-week training period including five training sessions, smokers in the avoidance-AAT trained to implicitly avoid all smoking-related cues, while smokers in the inhibition-AAT trained to implicitly inhibit behavioral response to smoking cues. During sham training, no such contingencies appeared. Self-report and behavioral data were assessed before and after training. Cigarette smoking and nicotine dependence were also assessed at 4- and 12-week follow-ups. Results: At posttest, avoidance training was more effective in reducing daily smoking than inhibition training. However, this difference was no longer evident in follow-up assessments. All training conditions improved other smoking- and health-related outcomes. Neither training changed smoking-related approach biases or associations, but approach biases for smoking-unrelated pictures increased and Stroop interference decreased in all conditions. Smoking devaluation was also comparable in all groups. Conclusions: Avoidance training might be slightly more effective in reducing smoking than inhibitory training. Overall, however, all four training types yielded equivalent therapy and training effects. Hence, a clear preference for one type of training remains premature. [ABSTRACT FROM AUTHOR]

Published

2022

13. Abuse and dependence potential of sphingosine-1-phosphate (S1P) receptor modulators used in the treatment of multiple sclerosis: a review of literature and public data.

Author

Schoedel, Kerri A., Kolly, Carine, Gardin, Anne, Neelakantham, Srikanth, and Shakeri-Nejad, Kasra

Subjects

*FINGOLIMOD, *SPHINGOSINE-1-phosphate, *MULTIPLE sclerosis, *MEDICATION abuse, *LITERATURE reviews, *DRUG abuse, *NATALIZUMAB, *DRUG addiction, *SUBSTANCE abuse, *ESTROGEN antagonists, *TREATMENT effectiveness, *DRUGS, *PSYCHOPHARMACOLOGY

Abstract

Abuse and misuse of prescription drugs remains an ongoing concern in the USA and worldwide; thus, all centrally active new drugs must be assessed for abuse and dependence potential. Sphingosine-1-phosphate (S1P) receptor modulators are used primarily in the treatment of multiple sclerosis. Among the new S1P receptor modulators, siponimod, ozanimod, and ponesimod have recently been approved in the USA, European Union (EU), and other countries. This review of literature and other public data has been undertaken to assess the potential for abuse of S1P receptor modulators, including ozanimod, siponimod, ponesimod, and fingolimod, as well as several similar compounds in development. The S1P receptor modulators have not shown chemical or pharmacological similarity to known drugs of abuse; have not shown abuse or dependence potential in animal models for subjective effects, reinforcement, or physical dependence; and do not have adverse event profiles demonstrating effects of interest to individuals who abuse drugs (such as sedative, stimulant, mood-elevating, or hallucinogenic effects). In addition, no reports of actual abuse, misuse, or dependence were identified in the scientific literature for fingolimod, which has been on the market since 2010 (USA) and 2011 (EU). Overall, the data suggest that S1P receptor modulators are not associated with significant potential for abuse or dependence, consistent with their unscheduled status in the USA and internationally. [ABSTRACT FROM AUTHOR]

Published

2022

14. In Memoriam Roy W. Pickens 1939–2022.

Author

Katz, Jonathan L., Hatsukami, Dorothy, Henningfield, Jack E., and Gust, Steven W.

Subjects

*PSYCHOPHARMACOLOGY, *GINGIVA, *SUBSTANCE-induced disorders, *DOPAMINE receptors, *DRUG addiction, *MEDICAL research, *COCAINE, *DRUG abuse treatment

Abstract

Dr. Pickens was remarkably productive during this time with more than 32 basic research papers on drug self-administration as well as 29 reviews and book chapters. In possibly the most influential of these papers, Pickens and Thompson ([6]) systematically studied the effects of cocaine dose and schedule of reinforcement on cocaine self-administration. Graph Roy W. Pickens died peacefully on May 25, 2022, at his home in Glen Allen, Virginia, where he and his wife Dace Svikis have lived since 1999. [Extracted from the article]

Published

2022

15. Editorial Special Issue on "Nature vs nurture in addiction research".

Author

Bradberry, Charles W and Baunez, Christelle

Subjects

*DRUG addiction, *NARCOTICS, *CLINICAL medicine research, *COCAINE, *PSYCHOPHARMACOLOGY

Published

2022

16. Intermittent but not continuous access to cocaine produces individual variability in addiction susceptibility in rats.

Author

Garcia, A. F., Webb, I. G., Yager, L. M., Seo, M. B., and Ferguson, S. M.

Subjects

*COCAINE, *DRUG addiction, *ADDICTIONS, *RATS, *INTRACELLULAR calcium, *CHRONIC diseases

Abstract

Drug addiction is a chronic disease defined by a complex set of characteristics, including loss of control over drug intake and persistent drug craving, which primarily affects a small percentage of people who try drugs. Although many models have been developed to study individual aspects of drug use, there is great translational value in having an animal model that encompasses multiple aspects of the human disease, including the variation in severity observed in humans. Here, we describe an intermittent access model of cocaine self-administration that produces a subset of rats that display many of the core features of addiction, including escalation of drug intake, a binge-like pattern of drug use, robust locomotor sensitization, and high levels of drug-seeking during cue-induced reinstatement. This group is compared with rats that have the same drug history but do not develop this pattern of drug-taking and drug-seeking, as well as rats that undergo a traditional continuous access paradigm. Finally, we observe that high levels of cocaine consumption produce long-term changes in intracellular calcium signaling in the dorsomedial striatum. [ABSTRACT FROM AUTHOR]

Published

2020

17. The role of HINT1 in methamphetamine-induced behavioral sensitization.

Author

Liu, Peng, Lei, Gang, Chu, Zheng, Deng, Li-sha, Yang, Liu, He, Jun-liang, and Dang, Yong-hui

Subjects

*METHAMPHETAMINE, *KNOCKOUT mice, *COMPULSIVE behavior, *DRUG addiction, *GEOMETRIC distribution, *HIP fractures, *NUCLEUS accumbens

Abstract

Background: Drug addiction is a chronically relapsing disorder in humans yet the underlying mechanism remained unclear. Recent studies suggested that histidine triad nucleotide binding protein1 (HINT1) may play significant roles in diverse neuropsychiatric diseases including drug addiction. Methods: In the current study, we used different batches of mice to establish different stages of methamphetamine (METH)-induced behavioral sensitization (BS) to explore the dynamic changes throughout the process of addiction in different brain regions, including the prefrontal cortex (PFC), nucleus accumbens (NAc), caudate putamen (CPu), and hippocampus (Hip). In addition, we used HINT1 knockout (KO) mice to investigate the effect of HINT1 protein deletion on METH-induced BS. Results: We found that in PFC of the METH group mice, the HINT1 expression level initially increased after development phase, and then dropped to the normal level during expression phase. However, there was no statistical difference in the HINT1 expression level in the other three encephalic regions (NAc, CPu, and Hip). The absence of HINT1 could promote METH-mediated addictive behavior to a certain extent, while the significant difference between genotypes only occurred in the development phase. Conclusions: Using the new technique, hip fractures were correctly predicted in 78% of cases compared with 36% when using the T-score. The accuracy of the prediction was not greatly reduced when using SSM and SAM (78% and 74% correct, respectively). Various geometric and BMD distribution traits were identified in the fractured and non-fractured groups. [ABSTRACT FROM AUTHOR]

Published

2020

18. Amitifadine, a triple reuptake inhibitor, reduces self-administration of the opiate remifentanil in rats.

Author

Levin, Edward D., Wells, Corinne, Hawkey, Andrew, Holloway, Zade, Blair, Graham, Vierling, Alexander, Ko, Ashley, Pace, Caroline, Modarres, John, McKinney, Anthony, Rezvani, Amir H., and Rose, Jed E.

Subjects

*REMIFENTANIL, *NARCOTICS, *DOPAMINE uptake inhibitors, *RATS, *DRUG addiction

Abstract

Rationale: A variety of neural systems are involved in drug addiction, and some of these systems are shared across different addictive drugs. We have found several different types of drug treatments that successfully reduce nicotine self-administration. Objectives: The current set of studies is the first in a series to determine if drug treatments that have been found to significantly reduce nicotine self-administration would reduce opiate self-administration. Methods: Amitifadine, a triple reuptake inhibitor of dopamine, norepinephrine, and serotonin, was assessed in female Sprague-Dawley rats to determine whether it significantly reduces remifentanil self-administration with either acute or chronic treatment. Results: Acutely, amitifadine doses of 5, 10, and 20 mg/kg each significantly reduced remifentanil self-administration. In a chronic study, repeated treatment with 10 mg/kg of amitifadine continued to reduce remifentanil self-administration, even after the cessation of treatment. However, amitifadine was not found to attenuate the rise in remifentanil self-administration with continued access. This study and our earlier one showed that the 10 mg/kg amitifadine dose did not significantly affect food motivated responding. Amitifadine did not attenuate remifentanil-induced antinociception as measured on the hot plate test but extended and maintained antinociceptive effects. Conclusions: These studies show the promise of amitifadine as a treatment for countering opiate self-administration for adjunctive use with opioids for analgesia. Further studies are needed to determine the possible efficacy of amitifadine for combating opiate addiction or preventing it in humans during adjunctive use with opioids for chronic pain. [ABSTRACT FROM AUTHOR]

Published

2020

19. Emergence of negative affect as motivation for drug taking in rats chronically self-administering cocaine.

Author

Klein, Samuel D., Beacher, Nicholas J., Kulik, Julianna M., Estrin, David J., Pawlak, Anthony P., and West, Mark O.

Subjects

*COCAINE, *VETERINARY drugs, *DRUGS of abuse, *DRUG addiction, *DRUG utilization

Abstract

Rationale: The role of negative affect as a motivational factor in animal models of drug addiction has been underexplored in the context of cocaine self-administration. Objectives: The present investigation studied the relationship between magnitude of affective response and quantity of cocaine consumed in order to clarify the affective components that drive drug use in a preclinical model. Methods: Rats self-administered (SA) cocaine 6 h/day for 14 consecutive days while their ultrasonic vocalizations (USVs) were recorded. Results: Animals displayed an increase in 50-kHz call rates (indicating positive affect) when their drug levels were rapidly rising and an increase in 22-kHz call rates (indicating negative affect) when forced to abstain. The rate of 50-kHz calls predicted drug consumption during the 1st week of SA, but not week two. Contrarily, there was a strongly predictive positive association between rate of 22-kHz calls and amount of drug consumed during the 2nd week of SA. Conclusions: Experimental results indicate that after chronic cocaine self-administration, negative affect emerges when animals are deprived of expected drug during withdrawal. Moreover, the increase in USVs indicating negative affect when deprived of drug was directly related to drug intake, concurrent with a decay in the direct relationship between USVs indicating positive affect and drug intake. The present preclinical support for the widely hypothesized shift from positive to negative affect as a salient motivational factor in human drug abuse adds to growing evidence of the unique value of rat USVs for understanding the role of emotion in drug addiction. [ABSTRACT FROM AUTHOR]

Published

2020

20. THC exposure during adolescence does not modify nicotine reinforcing effects and relapse in adult male mice.

Author

Flores, África, Maldonado, Rafael, and Berrendero, Fernando

Subjects

*NICOTINE, *ADOLESCENCE, *MICE, *ANIMAL behavior, *DRUG addiction, *OPERATIVE surgery, *NICOTIANA

Abstract

Rationale: Cannabis use is typically initiated during adolescence, and different studies suggest that adolescent cannabinoid exposure may increase the risk for drug addiction in adulthood. Objectives: This study investigated the effects of adolescent exposure to the main psychoactive component of cannabis, ∆9-tetrahydrocannabinol (THC), in the reinforcing properties of nicotine in adult male mice. Possible alterations in relapse to nicotine-seeking behaviour in adult animals due to THC adolescent exposure were also evaluated. Methods: Adolescent mice were exposed to escalating doses of THC from PND35 to PND49. When mice reached adulthood (PND70), surgical procedures were applied for further behavioural evaluation. Nicotine self-administration sessions were conducted consecutively for 10 days. Following extinction, mice were tested for cue- and stress-induced reinstatement of nicotine-seeking behaviour. Results: Adolescent THC treatment did not modify acquisition and extinction of nicotine self-administration in adulthood. Moreover, THC exposure did not alter relapse to nicotine seeking induced by stress or nicotine-associated cues. Conclusions: These results suggest that a history of exposure to THC during adolescence under these particular conditions does not modify the reinforcing effects and seeking behaviour of nicotine in the adult period. [ABSTRACT FROM AUTHOR]

Published

2020

21. The impact of cocaine and heroin drug history on motivation and cue sensitivity in a rat model of polydrug abuse.

Author

Crummy, Elizabeth A., Donckels, Elizabeth A., Baskin, Britahny M., Bentzley, Brandon S., and Ferguson, Susan M.

Subjects

*HEROIN, *COCAINE, *VETERINARY drugs, *LABORATORY rats, *MOTIVATION (Psychology), *DRUG abuse

Abstract

Rationale: Comorbid use of heroin and cocaine is highly prevalent among drug users and can greatly increase addiction risk. Nonetheless, little is known regarding how a multi-drug history impacts motivation and cue responsivity to individual drugs. Objective: We used behavioral-economic procedures to examine motivation to maintain drug consumption and tests of drug-seeking to drug-associated cues to assess sensitivity to heroin and cocaine-associated cues in rats that had a self-administration history of heroin, cocaine, or both drugs. Results: Unexpectedly, we found that groups with a polydrug history of heroin and cocaine did not have higher levels of motivation or cue-induced reinstatement of drug-seeking for either cocaine or heroin compared to single drug groups. Nonetheless, we did find drug-specific differences in both economic price and cue sensitivity. Specifically, demand elasticity was lower for cocaine compared to heroin in animals with a single drug history, but not with polydrug groups. In addition, cocaine demand was predictive of the degree of cue-induced reinstatement of drug-seeking for cocaine following extinction, whereas heroin demand was predictive of the degree of reactivity to a heroin-associated cue. Furthermore, although cue reactivity following the initial self-administration phase did not differ across cues and drug history, reactivity to both heroin and cocaine cues was greater during subsequent heroin use compared to cocaine use, and this enhanced reactivity to heroin cues persisted during forced abstinence. Conclusions: These results indicate that there is a greater motivation to maintain cocaine consumption, but higher sensitivity to drug-associated cues with a history of heroin use, suggesting that cocaine and heroin may drive continued drug use through different behavioral processes. [ABSTRACT FROM AUTHOR]

Published

2020

22. Special issue on conditioned determinants of reward seeking: a tribute to Dr. Nadia Chaudhri.

Author

Janak, Patricia H. and Shaham, Yavin

Subjects

*DRUG addiction, *ALCOHOL

Published

2023

23. Psychopathological symptoms associated with synthetic cannabinoid use: a comparison with natural cannabis.

Author

Mensen, Vincent T., Vreeker, Annabel, Nordgren, Johan, Atkinson, Amanda, de la Torre, Rafael, Farré, Magi, Ramaekers, Johannes G., and Brunt, Tibor M.

Subjects

*SUBSTANCE-induced disorders, *CANNABINOIDS, *BRIEF Symptom Inventory, *DRUG addiction, *MEDICAL marijuana, *SYNTHETIC marijuana, *MARIJUANA growing

Abstract

Background: Synthetic cannabinoids (SCs) are a class of new psychoactive substances that have been rapidly evolving around the world throughout recent years. Many different synthetic cannabinoid analogues are on the consumer market and sold under misleading names, like "spice" or "incense." A limited number of studies have reported serious health effects associated with SC use. In this study, we compared clinical and subclinical psychopathological symptoms associated with SC use and natural cannabis (NC) use. Methods: A convenience sample of 367 NC and SC users was recruited online, including four validated psychometric questionnaires: The Drug Use Disorders Identification Test (DUDIT), Insomnia Severity Index (ISI), Altman Mania Scale (Altman), and Brief Symptom Inventory (BSI). The two groups were compared with analysis of variance (ANOVA) and covariance (ANCOVA), chi2 tests, and logistic regression when appropriate. Results: The SC user group did not differ in age from the NC user group (27.7 years), but contained less females (21% and 30%, respectively). SC users scored higher than NC users on all used psychometric measures, indicating a higher likelihood of drug abuse, sleep problems, (hypo)manic symptoms, and the nine dimensions comprising the BSI, somatization, obsessive-compulsive behavior, interpersonal sensitivity, depression, anxiety, hostility, phobic anxiety, paranoid ideation, and psychoticism. Odds ratios (95% CI) for the SC user group vs NC user group were, respectively, drug dependence 3.56 (1.77–7.16), (severe) insomnia 5.01 (2.10–11.92), (hypo-)mania 5.18 (2.04–13.14), and BSI psychopathology 5.21 (2.96–9.17). Discussion: This study shows that SC use is associated with increased mental health symptomatology compared to NC use. [ABSTRACT FROM AUTHOR]

Published

2019

24. Impairments in reinforcement learning do not explain enhanced habit formation in cocaine use disorder.

Author

Lim, T. V., Cardinal, R. N., Savulich, G., Jones, P. S., Moustafa, A. A., Robbins, T. W., and Ersche, K. D.

Subjects

*COCAINE-induced disorders, *REINFORCEMENT learning, *COCAINE abuse, *PSYCHOLOGICAL feedback, *ACTION theory (Psychology), *DRUG addiction

Abstract

Rationale: Drug addiction has been suggested to develop through drug-induced changes in learning and memory processes. Whilst the initiation of drug use is typically goal-directed and hedonically motivated, over time, drug-taking may develop into a stimulus-driven habit, characterised by persistent use of the drug irrespective of the consequences. Converging lines of evidence suggest that stimulant drugs facilitate the transition of goal-directed into habitual drug-taking, but their contribution to goal-directed learning is less clear. Computational modelling may provide an elegant means for elucidating changes during instrumental learning that may explain enhanced habit formation. Objectives: We used formal reinforcement learning algorithms to deconstruct the process of appetitive instrumental learning and to explore potential associations between goal-directed and habitual actions in patients with cocaine use disorder (CUD). Methods: We re-analysed appetitive instrumental learning data in 55 healthy control volunteers and 70 CUD patients by applying a reinforcement learning model within a hierarchical Bayesian framework. We used a regression model to determine the influence of learning parameters and variations in brain structure on subsequent habit formation. Results: Poor instrumental learning performance in CUD patients was largely determined by difficulties with learning from feedback, as reflected by a significantly reduced learning rate. Subsequent formation of habitual response patterns was partly explained by group status and individual variation in reinforcement sensitivity. White matter integrity within goal-directed networks was only associated with performance parameters in controls but not in CUD patients. Conclusions: Our data indicate that impairments in reinforcement learning are insufficient to account for enhanced habitual responding in CUD. [ABSTRACT FROM AUTHOR]

Published

2019

25. A potential role for the gut microbiome in substance use disorders.

Author

Meckel, Katherine R. and Kiraly, Drew D.

Subjects

*SUBSTANCE-induced disorders, *HUMAN experimentation, *THERAPEUTICS, *VETERINARY drugs, *DRUG addiction, *GUT microbiome

Abstract

Pathological substance use disorders represent a major public health crisis with limited effective treatment options. While much work has been done to understand the neuronal signaling networks and intracellular signaling cascades associated with prolonged drug use, these studies have yielded few successful treatment options for substance use disorders. In recent years, there has been a growing interest to explore interactions between the peripheral immune system, the gut microbiome, and the CNS. In this review, we will present a summary of existing evidence, suggesting a potential role for gut dysbiosis in the pathogenesis of substance use disorders. Clinical evidence of gut dysbiosis in human subjects with substance use disorder and preclinical evidence of gut dysbiosis in animal models of drug addiction are discussed in detail. Additionally, we examine how changes in the gut microbiome and its metabolites may not only be a consequence of substance use disorders but may in fact play a role in mediating behavioral response to drugs of abuse. While much work still needs to be done, understanding the interplay of gut microbiome in substance use disorders may offer a promising avenue for future therapeutic development. [ABSTRACT FROM AUTHOR]

Published

2019

26. Heroin versus cocaine: opposite choice as a function of context but not of drug history in the rat.

Author

De Luca, Maria Teresa, Montanari, Christian, Meringolo, Maria, Contu, Laura, Celentano, Michele, and Badiani, Aldo

Subjects

*HEROIN, *COCAINE, *RATS, *DRUG addiction, *NARCOTICS

Abstract

Rationale: Previous studies have shown that rats trained to self-administer heroin and cocaine exhibit opposite preferences, as a function of setting, when tested in a choice paradigm. Rats tested at home prefer heroin to cocaine, whereas rats tested outside the home prefer cocaine to heroin. Here, we investigated whether drug history would influence subsequent drug preference in distinct settings. Based on a theoretical model of drug-setting interaction, we predicted that regardless of drug history rats would prefer heroin at home and cocaine outside the home.Methods: Rats with double-lumen catheters were first trained to self-administer either heroin (25 μg/kg) or cocaine (400 μg/kg) for 12 consecutive sessions. Twenty-six rats were housed in the self-administration chambers (thus, they were tested at home), whereas 30 rats lived in distinct home cages and were transferred to self-administration chambers only for the self-administration session (thus, they were tested outside the home). The rats were then allowed to choose repeatedly between heroin and cocaine within the same session for seven sessions.Results: Regardless of the training drug, the rats tested outside the home preferred cocaine to heroin, whereas the rats tested at home preferred heroin to cocaine. There was no correlation between drug preference and drug intake during the training phase.Conclusion: Drug preferences were powerfully influenced by the setting but, quite surprisingly, not by drug history. This suggests that, under certain conditions, associative learning processes and drug-induced neuroplastic adaptations play a minor role in shaping individual preferences for one drug or the other. [ABSTRACT FROM AUTHOR]

Published

2019

27. The emerging neuroscience of appetitive and drug cue extinction in humans.

Author

Konova, Anna B. and Goldstein, Rita Z.

Subjects

*EXTINCTION (Psychology), *FEAR, *ANXIETY disorders, *DRUG addiction, *PREFRONTAL cortex, *PROMPTS (Psychology), *NEUROSCIENCES, *PATHOLOGICAL psychology

Abstract

Fear extinction has been extensively studied in both humans and non-human animals, and this work has contributed greatly to our understanding and treatment of anxiety disorders. Yet other psychopathologies like addiction might be associated with impairments selectively in extinction of non-fear based, appetitive and drug cue associations, and these processes have been underexplored in clinical translational neuroscience. Important questions regarding similarities and differences in the neurobiological mechanisms underlying aversive and appetitive extinction remain unanswered, particularly those pertaining to cross-species evidence for the role of the ventromedial prefrontal cortex and, to some extent, the striatum. Here, we aim to draw attention to the paucity of studies investigating non-fear based extinction in humans, summarize emerging findings from the available literature, and highlight important directions for future research. We argue that closing these gaps in our understanding could help inform the development of more targeted, and perhaps more durable, forms of extinction-based treatments for addiction and related psychopathologies characterized by abnormally persistent appetitive and drug cue associations. [ABSTRACT FROM AUTHOR]

Published

2019

28. Role of prefrontal cortex in the extinction of drug memories.

Author

Zhang, Wen-Hua, Cao, Ke-Xin, Ding, Zeng-Bo, Yang, Jian-Li, Pan, Bing-Xing, and Xue, Yan-Xue

Subjects

*PREFRONTAL cortex, *EXTINCTION (Psychology), *MEMORY, *SUBSTANCE abuse relapse, *DRUG addiction, *PROMPTS (Psychology), *NEUROPLASTICITY, *NEURAL circuitry

Abstract

It has been recognized that drug addiction engages aberrant process of learning and memory, and substantial studies have focused on developing effective treatment to erase the enduring drug memories to reduce the propensity to relapse. Extinction, a behavioral intervention exposing the individuals to the drug-associated cues repeatedly, can weaken the craving and relapse induced by drug-associated cues, but its clinic efficacy is limited. A clear understanding of the neuronal circuitry and molecular mechanism underlying extinction of drug memory will facilitate the successful use of extinction therapy in clinic. As a key component of mesolimbic system, medial prefrontal cortex (mPFC) has received particular attention largely in that PFC stands at the core of neural circuits for memory extinction and manipulating mPFC influences extinction of drug memories and subsequent relapse. Here, we review the recent advances in both animal models of drug abuse and human addicted patients toward the understanding of the mechanistic link between mPFC and drug memory, with particular emphasis on how mPFC contributes to the extinction of drug memory at levels ranging from neuronal architecture, synaptic plasticity to molecular signaling and epigenetic regulation, and discuss the clinic relevance of manipulating the extinction process of drug memory to prevent craving and relapse through enhancing mPFC function. [ABSTRACT FROM AUTHOR]

Published

2019

29. Oprm1 A112G, a single nucleotide polymorphism, alters expression of stress-responsive genes in multiple brain regions in male and female mice.

Author

Collins, Devon, Randesi, Matthew, da Rosa, Joel Correa, Zhang, Yong, and Kreek, Mary Jeanne

Subjects

*OPIOID receptors, *GENETIC polymorphisms, *NUCLEUS accumbens, *DRUG addiction, *GENE expression

Abstract

Background: OPRM1 A118G, a functional human mu-opioid receptor (MOR) polymorphism, is associated with drug dependence and altered stress responsivity in humans as well as altered MOR signaling. MOR signaling can regulate many cellular processes, including gene expression, and many of the long-term, stable effects of drugs and stress may stem from changes in gene expression in diverse brain regions. A mouse model bearing an equivalent polymorphism (Oprm1 A112G) was previously generated and studied. Mice homozygous for the G112 allele show differences in opioid- and stress-related phenotypes.Approach: The current study examines the expression of 24 genes related to drug and stress responsivity in the caudoputamen, nucleus accumbens, hypothalamus, hippocampus, and amygdala of drug-naïve, stress-minimized, male and female mice homozygous for either the G112 variant allele or the wild-type A112 allele.Results: We detected nominal genotype-dependent changes in gene expression of multiple genes. We also detected nominal sex-dependent as well as sex-by-genotype interaction effects on gene expression. Of these, four genotype-dependent differences survived correction for multiple testing: Avp and Gal in the hypothalamus and Oprl1 and Cnr1 in the hippocampus.Conclusions: Changes in the regulation of these genes by mu-opioid receptors encoded by the G112 allele may be involved in some of the behavioral and molecular consequences of this polymorphism observed in mice. [ABSTRACT FROM AUTHOR]

Published

2018

30. Acute drug effects on habitual and non-habitual responding in crossed high alcohol preferring mice.

Author

Houck, Christa A. and Grahame, Nicholas J.

Subjects

*DRUG abuse, *ALCOHOLISM, *DRUG addiction, *SUBSTANCE abuse, *ALCOHOLIC intoxication

Abstract

Rationale: Drug reward plays a central role in acquiring drug-seeking behavior. However, subjects may continue using drugs despite negative consequences because self-administration becomes habitual, and divorced from outcome values. Although a history of drug and alcohol use expedite habit acquisition, and in spite of the fact that self-administration leads to intoxication, the acute effects of drugs on habitual responding are not well understood.Objectives: We sought to observe how acute ethanol and amphetamine affect the balance between habitual and goal-directed behavior, as measured by a fluid-reinforced operant conditioning task.Methods: Selectively bred crossed high-alcohol-preferring (cHAP) mice were trained on an operant conditioning task reinforced on a variable interval schedule with 1% banana solution, which was subsequently devalued via LiCl pairing in half the animals. Ethanol (1.0 g/kg), amphetamine (2.0 mg/kg), or saline was administered prior to a post-devaluation test.Results: Overall, mice showed habitual behavior, but when divided into high- or low-responding groups based on training response rates, saline-treated, low-responding animals devalued, while saline-treated high-responding animals did not. Furthermore, amphetamine elicited devaluation even in high-responding animals, while ethanol prevented devaluation even in low-responding animals.Conclusions: These data show that ethanol shifts animals toward behaving habitually. This may illuminate why alcohol-intoxicated individuals display impaired judgment about the relative merits of drinking, and potentially serve as a mechanism by which intoxicated subjects resume previously devalued behaviors, such as comorbid drug use. These findings also show that high variable interval response rates facilitate a shift from goal-directed to habitual behavior. [ABSTRACT FROM AUTHOR]

Published

2018

31. Different functional domains measured by cocaine self-administration under the progressive-ratio and punishment schedules in male Wistar rats.

Author

Datta, Udita, Martini, Mariangela, and WenLin Sun

Subjects

*COCAINE, *PUNISHMENT, *COCAINE abuse, *RESPONSE inhibition, *DRUG addiction, *RATS, *SYMPTOMS

Abstract

Background Current diagnosis of drug addiction like other mental disorders is based on clinical symptoms not on neural pathophysiology and consequently, does not provide useful information on the underlying pathophysiology and may impede the efforts to identify the underlying mechanisms. Identifying the functional deficits that are relevant to addiction and can be traced to the neural systems will greatly facilitate our understanding of the heterogeneity of the condition and improve future diagnosis and treatment. Cocaine addiction is characterized by the continued use despite the dire consequences, and the deficit in inhibitory control may play a key role in this process. This study aimed to develop a paradigm to measure the punishmentinduced inhibitory regulation of reward-seeking behavior. Methods Rats were first trained to self-administer sucrose pellets under a chained schedule and then the breaking points (BPs) under the progressive-ratio schedule, and the intensity-response effects of footshock punishment on sucrose SA were measured. Subsequently, the rats went on to self-administer intravenous cocaine, and the BPs and the punishment intensity-response effects were similarly determined. Results The areas under the punishment intensity-response curves (AUCs) were calculated and used as an indicator of the sensitivity of the inhibitory system. The BPs for cocaine were not correlated with the AUCs. Furthermore, the change in the BPs for cocaine induced by changing cocaine dose did not predict the change in the AUCs. Conclusion The intensity-response effects of punishment can be used to measure the function or sensitivity of the inhibitory system independent of the motivational state. [ABSTRACT FROM AUTHOR]

Published

2018

32. Sex-specific attenuation of impulsive action by progesterone in a go/no-go task for cocaine in rats.

Author

Swalve, Natashia, Smethells, John R., Younk, Rebecca, Mitchell, Jared, Dougen, Ben, and Carroll, Marilyn E.

Subjects

*COCAINE & psychology, *PROGESTERONE, *IMPULSE (Psychology), *BIOCHEMICAL mechanism of action, *LABORATORY rats

Abstract

Rationale: Previous work indicated that progesterone (PRO) reduced impulsive choice for cocaine in female but not male rats (Smethells et al. Psychopharmacology 233:2999-3008, 2016). Impulsive action, typically measured by responding for a reinforcer during a signaled period of nonavailability of natural reinforcers, predicts initiation and escalation of drug use in animals and humans. The present study examined impulsive action for cocaine using PRO in male and female rats trained on a go/no-go task. Objective: Rats were trained on a go/no-go task to respond for cocaine infusions (0.4 mg/kg/inf). During the 'go' component, responding was reinforced on a VI 30-s schedule, whereas during the 'no-go' component, withholding a response was reinforced on a differential reinforcement of other behavior (DRO) 30-s schedule. A response during the no-go component resets the DRO timer and served as a measure of impulsive action. After baseline responding was established, rats were pretreated with vehicle (VEH) or PRO (0.5 mg/kg), and DRO resets and responding during the go component for cocaine were compared in males vs. females. Results: DRO resets were significantly lower following PRO treatment compared to VEH in female, but not male, rats. Response rates and overall infusions during the go component were not significantly altered by PRO in either females or males. Conclusion: Treatment with PRO resulted in a sex-specific reduction in impulsive action for cocaine, while not affecting cocaine self-administration. [ABSTRACT FROM AUTHOR]

Published

2018

33. High and escalating levels of cocaine intake are dissociable from subsequent incentive motivation for the drug in rats.

Author

Allain, Florence, Bouayad-Gervais, Karim, and Samaha, Anne-Noël

Subjects

*COCAINE, *DRUG addiction, *DISSOCIATION (Psychology), *DRUG administration, *LABORATORY rats, *PHYSIOLOGY

Abstract

Rationale: Taking high and increasing amounts of cocaine is thought to be necessary for the development of addiction. Consequently, a widely used animal model of drug self-administration involves giving animals continuous drug access during long sessions (LgA), as this produces high and escalating levels of intake. However, human cocaine addicts likely use the drug with an intermittent rather than continuous pattern, producing spiking brain cocaine levels. Objectives: Using an intermittent-access (IntA) cocaine self-administration procedure in rats, we studied the relationship between escalation of cocaine intake and later incentive motivation for the drug, as measured by responding under a progressive ratio schedule of cocaine reinforcement. Results: First, under IntA, rats escalated their cocaine use both within and between sessions. However, escalation did not predict later incentive motivation for the drug. Second, incentive motivation for cocaine was similar in IntA-rats limited to low- and non-escalating levels of drug intake (IntA-Lim) and in IntA-rats that took high and escalating levels of drug. Finally, IntA-Lim rats took much less cocaine than rats given continuous drug access during each self-administration session (LgA-rats). However, IntA-Lim rats later responded more for cocaine under a progressive ratio schedule of reinforcement. Conclusions: Taking large and escalating quantities of cocaine does not appear necessary to increase incentive motivation for the drug. Taking cocaine in an intermittent pattern-even in small amounts-is more effective in producing this addiction-relevant change. Thus, beyond the amount of drug taken, the temporal kinetics of drug use predict change in drug use over time. [ABSTRACT FROM AUTHOR]

Published

2018

34. Steep effort discounting of a preferred reward over a freely-available option in prolonged methamphetamine withdrawal in male rats.

Author

Thompson, Andrew, Gerson, Julian, Stolyarova, Alexandra, Bugarin, Amador, Hart, Evan, Jentsch, J., and Izquierdo, Alicia

Subjects

*DRUG addiction, *LABORATORY rats, *METHAMPHETAMINE, *METHAMPHETAMINE abuse, *SUCROSE

Abstract

Rationale: Drug addiction can be described as aberrant allocation of effort toward acquiring drug, despite associated costs. It is unclear if this behavioral pattern results from an overvaluation of reward or to an altered sensitivity to costs. Objective: Present experiments assessed reward sensitivity and effortful choice in rats following 1 week of withdrawal from methamphetamine (mAMPH). Methods: Rats were treated with either saline or an escalating dose mAMPH regimen, then tested after a week without the drug. In experiment 1, rats were given a free choice between water and various concentrations of sucrose solution to assess general reward sensitivity. In experiment 2, rats were presented with a choice between lever-pressing for sucrose pellets on a progressive ratio schedule or consuming freely-available chow. Results: In experiment 1, we found no differences in sucrose preference between mAMPH- and saline-pretreated rats. In experiment 2, when selecting between two options, mAMPH-pretreated rats engaged in less lever-pressing for sucrose pellets ( p < 0.01) and switched from this preferred reward to the chow sooner than saline-pretreated rats ( p < 0.05). This effect was not consistent with general reward devaluation or loss of motivation. Conclusions: These findings demonstrate that mAMPH exposure and withdrawal lead to steeper discounting of reward value by effort, an effect that is consistent with the effect of mAMPH on discounting by delay, and which may reflect an underlying shared mechanism. [ABSTRACT FROM AUTHOR]

Published

2017

35. Atomoxetine effects on attentional bias to drug-related cues in cocaine dependent individuals.

Author

Passamonti, Luca, Luijten, M., Ziauddeen, H., Coyle-Gilchrist, I., Rittman, T., Brain, S., Regenthal, R., Franken, I., Sahakian, B., Bullmore, E., Robbins, T., and Ersche, K.

Subjects

*ATOMOXETINE, *COCAINE, *DRUG addiction, *PLACEBOS, *INHIBITORY postsynaptic potential

Abstract

Rationale: Biased attention towards drug-related cues and reduced inhibitory control over the regulation of drug-intake characterize drug addiction. The noradrenaline system has been critically implicated in both attentional and response inhibitory processes and is directly affected by drugs such as cocaine. Objectives: We examined the potentially beneficial effects of the noradrenaline reuptake inhibitor atomoxetine in improving cognitive control during two tasks that used cocaine- and non-cocaine-related stimuli. Methods: A double-blind, placebo-controlled, and cross-over psycho-pharmacological design was employed. A single oral dose of atomoxetine (40 mg) was administered to 28 cocaine-dependent individuals (CDIs) and 28 healthy controls. All participants performed a pictorial attentional bias task involving both cocaine- and non-cocaine-related pictures as well as a verbal go/no-go task composed of cocaine- and food-related words. Results: As expected, CDIs showed attentional bias to cocaine-related cues whilst controls did not. More importantly, however, atomoxetine, relative to placebo, significantly attenuated attentional bias in CDIs ( F = 6.73, P = 0.01). During the go/no-go task, there was a treatment × trial × group interaction, although this finding only showed a trend towards statistical significance ( F = 3.38, P = 0.07). Conclusions: Our findings suggest that atomoxetine reduces attentional bias to drug-related cues in CDIs. This may result from atomoxetine's modulation of the balance between tonic/phasic activity in the locus coeruleus and the possibly parallel enhancement of noradrenergic neurotransmission within the prefrontal cortex. Studying how cognitive enhancers such as atomoxetine influence key neurocognitive indices in cocaine addiction may help to develop reliable biomarkers for patient stratification in future clinical trials. [ABSTRACT FROM AUTHOR]

Published

2017

36. Cannabis-related hippocampal volumetric abnormalities specific to subregions in dependent users.

Author

Chye, Yann, Suo, Chao, Yücel, Murat, Ouden, Lauren, Solowij, Nadia, and Lorenzetti, Valentina

Subjects

*CANNABIS (Genus), *HIPPOCAMPUS diseases, *HUMAN abnormalities, *DRUG addiction, *DENTATE gyrus

Abstract

Rationale: Cannabis use is associated with neuroanatomical alterations in the hippocampus. While the hippocampus is composed of multiple subregions, their differential vulnerability to cannabis dependence remains unknown. Objectives: The objective of the study is to investigate gray matter alteration in each of the hippocampal subregions (presubiculum, subiculum, cornu ammonis (CA) subfields CA1-4, and dentate gyrus (DG)) as associated with cannabis use and dependence. Methods: A total of 35 healthy controls (HC), 22 non-dependent (CB-nondep), and 39 dependent (CB-dep) cannabis users were recruited. We investigated group differences in hippocampal subregion volumes between HC, CB-nondep, and CB-dep users. We further explored the association between CB use variables (age of onset of regular use, monthly use, lifetime use) and hippocampal subregions in CB-nondep and CB-dep users separately. Results: The CA1, CA2/3, CA4/DG, as well as total hippocampal gray matter were reduced in volume in CB-dep but not in CB-nondep users, relative to HC. The right CA2/3 and CA4/DG volumes were also negatively associated with lifetime cannabis use in CB-dep users. Conclusions: Our results suggest a regionally and dependence-specific influence of cannabis use on the hippocampus. Hippocampal alteration in cannabis users was specific to the CA and DG regions and confined to dependent users. [ABSTRACT FROM AUTHOR]

Published

2017

37. Orbitofrontal and caudate volumes in cannabis users: a multi-site mega-analysis comparing dependent versus non-dependent users.

Author

Chye, Yann, Solowij, Nadia, Suo, Chao, Batalla, Albert, Cousijn, Janna, Goudriaan, Anna, Martin-Santos, Rocio, Whittle, Sarah, Lorenzetti, Valentina, and Yücel, Murat

Subjects

*CANNABIS (Genus), *PHYSIOLOGY, *BRAIN physiology, *BRAIN function localization, *DRUG addiction, *MAGNETIC resonance imaging

Abstract

Rationale: Cannabis (CB) use and dependence are associated with regionally specific alterations to brain circuitry and substantial psychosocial impairment. Objectives: The objective of this study was to investigate the association between CB use and dependence, and the volumes of brain regions critically involved in goal-directed learning and behaviour-the orbitofrontal cortex (OFC) and caudate. Methods: In the largest multi-site structural imaging study of CB users vs healthy controls (HC), 140 CB users and 121 HC were recruited from four research sites. Group differences in OFC and caudate volumes were investigated between HC and CB users and between 70 dependent (CB-dep) and 50 non-dependent (CB-nondep) users. The relationship between quantity of CB use and age of onset of use and caudate and OFC volumes was explored. Results: CB users (consisting of CB-dep and CB-nondep) did not significantly differ from HC in OFC or caudate volume. CB-dep compared to CB-nondep users exhibited significantly smaller volume in the medial and the lateral OFC. Lateral OFC volume was particularly smaller in CB-dep females, and reduced volume in the CB-dep group was associated with higher monthly cannabis dosage. Conclusions: Smaller medial OFC volume may be driven by CB dependence-related mechanisms, while smaller lateral OFC volume may be due to ongoing exposure to cannabinoid compounds. The results highlight a distinction between cannabis use and dependence and warrant examination of gender-specific effects in studies of CB dependence. [ABSTRACT FROM AUTHOR]

Published

2017

38. Don't stress about CRF: assessing the translational failures of CRFantagonists.

Author

Spierling, Samantha and Zorrilla, Eric

Subjects

*CORTICOTROPIN releasing hormone, *MENTAL depression, *DRUG addiction, *NEUROBIOLOGY, *HUMAN genetics

Abstract

Background: Dr. Athina Markou sought treatments for a common neural substrate shared by depression and drug dependence. Antagonists of corticotropin-releasing factor (CRF) receptors, a target of interest to her, have not reached the clinic despite strong preclinical rationale and sustained translational efforts. Methods: We explore potential causes for the failure of CRF antagonists and review recent findings concerning CRF-CRF systems in psychopathology. Results: Potential causes for negative outcomes include (1) poor safety and efficacy of initial drug candidates due to bad pharmacokinetic and physicochemical properties, (2) specificity problems with preclinical screens, (3) the acute nature of screens vs. late-presenting patients, (4) positive preclinical results limited to certain models and conditions with dynamic CRF-CRF activation not homologous to tested patients, (5) repeated CRF activation-induced plasticity that reduces the importance of ongoing CRF agonist stimulation, and (6) therapeutic silencing which may need to address CRF receptor or CRF-binding protein molecules, constitutive CRF activity, or molecules that influence agonist-independent activity or to target structural regions other than the allosteric site bound by all drug candidates. We describe potential markers of activation towards individualized treatment, human genetic, and functional data that still implicate CRF systems in emotional disturbance, sex differences, and suggestive clinical findings for CRF antagonists in food craving and CRF-driven HPA-axis overactivation. Conclusion: The therapeutic scope of selective CRF antagonists now appears narrower than had been hoped. Yet, much remains to be learned about CRF's role in the neurobiology of dysphoria and addiction and the potential for novel anti-CRF therapies therein. [ABSTRACT FROM AUTHOR]

Published

2017

39. A comparison of psychotic symptoms in subjects with methamphetamine versus cocaine dependence.

Author

Alexander, Peter, Gicas, Kristina, Willi, Taylor, Kim, Clara, Boyeva, Veronika, Procyshyn, Ric, Smith, Geoff, Thornton, Allen, Panenka, William, Jones, Andrea, Vila-Rodriguez, Fidel, Lang, Donna, William MacEwan, G, Honer, William, and Barr, Alasdair

Subjects

*PSYCHOSES, *METHAMPHETAMINE, *DRUG addiction, *COGNITION, *DOPAMINE agonists

Abstract

Rationale: The psychostimulant drugs cocaine and methamphetamine are potent indirect dopamine receptor agonists which act through similar but not identical mechanisms. Studies in humans have observed that a large proportion of those who chronically use these drugs experience psychotic symptoms. However, direct comparisons of psychotic symptom severity between cocaine and methamphetamine users are lacking. Objectives: The goal of the present study was to directly compare severity of psychotic symptoms between cocaine- and methamphetamine-dependent individuals. Additionally, we sought to determine how concurrent cocaine + methamphetamine dependence would influence psychotic symptoms. Methods: We recruited 153 polysubstance-using subjects meeting DSM-IV-TR criteria for cocaine dependence, 38 with methamphetamine dependence, and 32 with cocaine + methamphetamine dependence. Psychotic symptoms were assessed with the Positive and Negative Syndrome Scale (PANSS) and analyzed using a five-factor model. All participants were also assessed for physical and mental illnesses as well as recent substance use. Most subjects completed a comprehensive neurocognitive battery. Results: While all three groups exhibited high total PANSS scores, the positive symptom subscale was significantly higher in the methamphetamine-dependent (17.03 ± 6.3) than the cocaine-dependent group (13.51 ± 4.12) and non-significantly higher ( p = 0.08) than the cocaine + methamphetamine group (14.44 ± 5.50). Groups also differed on demographic variables, viral infection, and other indices of substance use, which were unlikely to account for the difference in positive symptoms. There were only modest differences between groups in neurocognitive function. Conclusions: Methamphetamine dependence was associated with more severe positive symptoms of psychosis than cocaine dependence. Concurrent cocaine + methamphetamine dependence did not increase psychosis severity. [ABSTRACT FROM AUTHOR]

Published

2017

40. mGlu1 receptor as a drug target for treatment of substance use disorders: time to gather stones together?

Author

Dravolina, Olga, Zvartau, Edwin, Danysz, Wojciech, and Bespalov, Anton

Subjects

*ALLOSTERIC regulation, *DRUG addiction, *DRUG abuse, *NEUROPLASTICITY, *NEUROPHYSIOLOGY

Abstract

Modulation of the mGlu1 receptor was repeatedly shown to inhibit various phenomena associated with exposure to abused drugs. Efficacy in preclinical models was observed with both positive and negative allosteric modulators (PAMs and NAMs, respectively) using essentially non-overlapping sets of experimental methods. Taken together, these data indicate that the mGlu1 receptor certainly plays a significant role in the plasticity triggered by the exposure to abused drugs and is involved in the maintenance of drug-seeking and drug-taking behaviors. Understanding whether modulation of the mGlu1 receptor activity can also affect drug-seeking and drug-taking in humans could have a significant impact on the future development of medications in this field. We argue that the mGlu1 receptor NAMs have a significant value as potential tools for human experimental pharmacology that could help to validate methods used in preclinical research. Compared with the PAMs, the mGlu1 receptor NAMs appear to be better candidates for this role due to the following: (1) a number of highly potent, selective, and chemically diverse mGlu1 receptor NAMs to choose from; (2) availability of high-quality PET ligands to monitor target exposure; and (3) a rich pharmacological profile with a number of effects that can complement anti-addictive action (e.g., anxiolytic/antidepressant) and may also serve as additional pharmacodynamic readouts during the preclinical-to-clinical translation. We believe that the mGlu1 receptor NAMs have a significant value as potential tools for human experimental pharmacology that could help to validate methods used in preclinical research. [ABSTRACT FROM AUTHOR]

Published

2017

41. Dopamine D1 and D3 receptor interactions in cocaine reward and seeking in rats.

Author

Galaj, E., Harding, W., and Ranaldi, R.

Subjects

*DOPAMINE receptors, *COCAINE, *LABORATORY rats, *DRUG addiction, *PEOPLE with drug addiction

Abstract

Rationale: Animal research has demonstrated a role of dopamine D1 and D3 receptors in cocaine reward and seeking. Purpose and methods: Here, we investigated the potential interaction of these two dopamine receptors in cue-induced reinstatement of cocaine seeking, cocaine conditioned place preference (CPP), and cocaine self-administration in rats. Results: The co-administration of a D3 receptor antagonist, NGB 2904 and a D1 partial agonist, SKF 77434, of doses which when administered individually produced no significant effects, prior to reinstatement or CPP tests significantly reduced lever pressing and time spent in the cocaine-paired environment, suggesting synergistic effects of the combined compounds on cocaine seeking. When given to rats self-administering cocaine under a progressive ratio schedule of reinforcement doses of NGB 2904 which were ineffective alone significantly enhanced the break point-reducing effects of SKF 77434. Conclusions: Our results indicate that the combined treatment with a D1 receptor partial agonist and D3 receptor antagonist produces robust decreases in cocaine seeking and reward. This suggests an interaction between dopamine D1 and D3 receptors in cocaine-related behaviors. [ABSTRACT FROM AUTHOR]

Published

2016

42. Metabolic shift of the kynurenine pathway impairs alcohol and cocaine seeking and relapse.

Author

Vengeliene, Valentina, Cannella, Nazzareno, Takahashi, Tatiane, and Spanagel, Rainer

Subjects

*KYNURENINE, *ALCOHOLISM relapse, *COCAINE, *DRUG development, *METHYL aspartate receptors, *DRUG addiction, *THERAPEUTICS

Abstract

Rationale: The glutamatergic system plays a key role in the maintenance of drug use and development of drug-related conditioned behaviours. In particular, hyper-glutamatergic activity and N-methyl-D-aspartate receptor (NMDAR) activation may drive drug craving and relapse. Inhibition of kynurenine-3-monooxygenase (KMO) shifts the metabolic kynurenine pathway towards production of kynurenic acid, which leads to a reduction of glutamatergic/NMDAR activity via different mechanisms. Objectives: In this study, we investigated whether drug-seeking and relapse behaviour could be modified by the metabolic shift of endogenous kynurenine pathway. Methods: An inhibitor of kynurenine-3-monooxygenase (KMO) Ro61-8048 (4 and 40 mg/kg) and its prodrug JM6 (100 and 200 mg/kg) were tested in two behavioural rat models for drug seeking and relapse-the alcohol deprivation effect (ADE) model in long-term alcohol-drinking rats and the model of cue-induced reinstatement of alcohol- and cocaine-seeking behaviour. Results: Our results show that relapse-like alcohol drinking during the ADE was abolished by repeated intraperitoneal administration of Ro61-8048 and significantly reduced by its oral prodrug JM6. Cue-induced reinstatement of both alcohol- and cocaine-seeking behaviour was also abolished by administration of Ro61-8048. Conclusions: Pharmacological enhancement of endogenous kynurenic acid levels provides a novel treatment strategy to interfere with glutamatergic/NMDAR activity as well as with craving and relapse in alcohol-dependent patients and drug addicts. [ABSTRACT FROM AUTHOR]

Published

2016

43. The tendency to sign-track predicts cue-induced reinstatement during nicotine self-administration, and is enhanced by nicotine but not ethanol.

Author

Versaggi, Cassandra, King, Christopher, and Meyer, Paul

Subjects

*NICOTINE addiction, *PROMPTS (Psychology), *REWARD (Psychology), *CHOLINERGIC receptors, *DESIRE, *EXTINCTION (Psychology)

Abstract

Rationale: Some individuals are particularly responsive to reward-associated stimuli ('cues'), including the effects of these cues on craving and relapse to drug-seeking behavior. In the cases of nicotine and alcohol, cues may acquire these abilities via the incentive-enhancing properties of the drug. Objectives: To determine the interaction between cue-responsivity and nicotine reinforcement, we studied the patterns of nicotine self-administration in rats categorized based on their tendency to approach a food-predictive cue ('sign-trackers') or a reward-delivery location ('goal-trackers'). In a second experiment, we determined whether nicotine and ethanol altered the incentive value of a food cue. Methods: Rats were classified as sign- or goal-trackers during a Pavlovian conditioned approach paradigm. Rats then self-administered intravenous nicotine (0.03 mg/kg infusions) followed by extinction and cue-induced reinstatement tests. We also tested the effects of nicotine (0.4 mg/kg base s.c.) or ethanol (0.7 g/kg i.p.) on the approach to, and reinforcing efficacy of, a food cue. Results: Sign-trackers showed greater reinstatement in response to a nicotine cue. Further, nicotine enhanced sign-tracking but not goal-tracking to a food cue and also enhanced responding for the food cue during the conditioned reinforcement test. Conversely, ethanol reduced sign-tracking and increased goal-tracking, but had no effect on conditioned reinforcement. Conclusions: Our studies demonstrate that the tendency to attribute incentive value to a food cue predicts enhanced cue-induced reinstatement. Additionally, the incentive value of food cues is differentially modulated by nicotine and ethanol, which may be related to the reinforcing effects of these drugs. [ABSTRACT FROM AUTHOR]

Published

2016

44. Delay and probability discounting by drug-dependent cocaine and marijuana users.

Author

Mejía-Cruz, Diana, Green, Leonard, Myerson, Joel, Morales-Chainé, Silvia, and Nieto, Javier

Subjects

*COCAINE, *PHYSIOLOGICAL effects of marijuana, *DRUG addiction, *FACTOR analysis, *TASK performance, *PHYSIOLOGY

Abstract

Rationale: Steep discounting of delayed monetary rewards by substance-dependent individuals is well-established. Less is known, however, about discounting other kinds of outcomes, and very little is known about discounting by marijuana-dependent individuals. Objectives: To determine how cocaine-dependent individuals and marijuana-dependent individuals discount various delayed and probabilistic outcomes, both positive and negative. Methods: Marijuana-dependent individuals, cocaine-dependent individuals, and controls performed delay and probability discounting tasks with various hypothetical outcomes. Results: The cocaine-dependent (but not the marijuana-dependent) group discounted delayed liquid rewards and monetary gains, but not delayed losses, more steeply than the control group. In contrast, the marijuana-dependent group (but not the cocaine-dependent group) discounted delayed monetary losses more steeply than controls. There were no group differences in discounting for any of the probabilistic outcomes. Factor analysis revealed a delayed gain factor, a probabilistic gain factor, and a delayed/probabilistic loss factor. The delayed gain factor scores for the cocaine-dependent group, but not the marijuana-dependent group, differed significantly from those of the control group. The groups did not differ in their probabilistic gain factor scores, and the marijuana-dependent group did not differ from the controls with respect to their loss factor scores. Conclusions: These results are inconsistent with the idea that steep discounting of both gains and losses and both delayed and probabilistic outcomes reflects a general impulsivity trait, as well as with the idea that all drug-dependent individuals are steep discounters. Rather, differences in discounting appear to be related to both the type of outcome and the specific drug on which individuals are dependent. [ABSTRACT FROM AUTHOR]

Published

2016

45. Premature responding is associated with approach to a food cue in male and female heterogeneous stock rats.

Author

King, Christopher, Palmer, Abraham, Woods, Leah, Hawk, Larry, Richards, Jerry, and Meyer, Paul

Subjects

*ATTENTION-deficit hyperactivity disorder, *TREATMENT of attention-deficit hyperactivity disorder, *DRUG addiction, *LABORATORY rats, *METHYLPHENIDATE

Abstract

Rationale: Disorders of behavioral regulation, including attention deficit hyperactivity disorder (ADHD) and drug addiction, are in part due to poor inhibitory control, attentional deficits, and hyper-responsivity to reward-associated cues. Objectives: To determine whether these traits are related, we tested genetically variable male and female heterogeneous stock rats in the choice reaction time (CRT) task and Pavlovian conditioned approach (PavCA). Sex differences in the response to methylphenidate during the CRT were also assessed. Methods: In the CRT task, rats were required to withhold responding until one of two lights indicated whether responses into a left or right port would be reinforced with water. Reaction time on correct trials and premature responses were the operational definitions of attention and response inhibition, respectively. Rats were also pretreated with oral methylphenidate (0, 2, 4 mg/kg) during the CRT task to determine whether this drug would improve performance. Subsequently, during PavCA, presentation of an illuminated lever predicted the delivery of a food pellet into a food-cup. Lever-directed approach (sign-tracking) and food-cup approach (goal-tracking) were the primary measures, and rats were categorized as 'sign-trackers' and 'goal-trackers' using an index based on these measures. Results: Sign-trackers made more premature responses than goal-trackers but showed no differences in reaction time. There were sex differences in both tasks, with females having higher sign-tracking, completing more CRT trials, and making more premature responses after methylphenidate administration. Conclusions: These results indicate that response inhibition is related to reward-cue responsivity, suggesting that these traits are influenced by common genetic factors. [ABSTRACT FROM AUTHOR]

Published

2016

46. Conditioned stimuli's role in relapse: preclinical research on Pavlovian-Instrumental-Transfer.

Author

Lamb, R., Schindler, Charles, and Pinkston, Jonathan

Subjects

*DRUG addiction, *INGESTION, *STIMULUS & response (Psychology), *MOTIVATION (Psychology), *LEARNING

Abstract

Rationale and objective: Pavlovian learning is central to many theories of addiction. In these theories, stimuli paired with drug ingestion become conditioned stimuli (CS) and subsequently elicit drug-seeking and drug-taking. However, in most relevant studies, Pavlovian and instrumental learning are confounded. This confound may be avoided in Pavlovian-Instrumental-Transfer (PIT) procedures. In PIT, Pavlovian and instrumental learning are established separately and then combined. In order to better understand the role of CSs in addiction, we review the relevant studies using PIT. Findings: We identified seven articles examining PIT effects of ethanol- or cocaine-paired CSs. Under at least one condition, six of these articles reported CS-elicited increases in responding previously maintained by drug. However, the only study using the optimal control condition failed to find a CS-elicited increase. Two studies examining CS specificity found the CS also increased responding maintained by a different reinforcer. Two studies examined if CSs elicit increases in actual drug-taking. Both failed to find CS-elicited increases, i.e., no study shows CS-elicited increases in actual drug-taking. Further, CS-elicited increases in extinguished responding are short-lived. Conclusions: These findings are not entirely consistent with Pavlovian learning playing a central role in addiction. However, design issues can explain most of these inconsistencies. Studies without these design issues are needed. Additionally, existing theories hypothesize drug-paired CSs increase drug-taking by increasing motivation, by eliciting conditioned responses that make drug-seeking more probable, or by a combination of these. Work distinguishing between these mechanisms would also be useful. [ABSTRACT FROM AUTHOR]

Published

2016

47. When the party is over: depressive-like states in rats following termination of cortical D1 receptor overexpression.

Author

Freund, Nadja, Thompson, Britta, Sonntag, Kai, Meda, Shirisha, and Andersen, Susan

Subjects

*MENTAL depression, *DOPAMINE receptors, *GENETIC overexpression, *BIPOLAR disorder, *DRUG addiction, *LABORATORY rats

Abstract

Rationale: Increased activity of prefrontal D1 dopamine receptors (D1R) is involved in reward-related behavior found in bipolar disorder and drug addiction. While the effects of elevated D1R are known, depressive-like behaviors also occur in these disorders after reward-seeking ends. Objectives: The goal is to characterize how termination of D1R overexpression influences depressive-like behaviors. Methods: An inducible (Tet.On), lentiviral vector was used to manipulate the expression of the DRD1 gene in glutamate neurons within the prefrontal cortex in male, adult rats. Sexual activity and sucrose preference were studied in both D1R elevated ON and relatively reduced OFF states. Following termination of the D1R ON state, depressive-like behavior was determined in the OFF state. Expression of the transcriptional regulator, cyclic AMP-responsive element-binding protein (CREB), was used as an indication of downstream effects in the nucleus accumbens (NA). Results: ON D1R expression increased sexual activity that returned to baseline in the OFF state. Sucrose preferences increased ~6 % in ON state but fell 11 % below control levels when OFF. Consistent with a depressive-like phenotype, D1R OFF decreased activity by 40 %, impaired the ability to control (43 %) and motivation to escape shock (27 % more impaired) relative to dsRed OFF. CREB increased 29 % in the NA in the D1R OFF state relative to the ON state. Conclusions: This novel approach demonstrates that elevated D1R expression increased hedonic behavior, whereas the termination of D1R overexpression often resulted in depressive-like behavior. These observations support a role for D1R expression cycling in bipolar-associated behaviors and addiction. [ABSTRACT FROM AUTHOR]

Published

2016

48. Sex differences in the acquisition and maintenance of cocaine and nicotine self-administration in rats.

Author

Swalve, Natashia, Smethells, John, and Carroll, Marilyn

Subjects

*COCAINE, *NICOTINE, *DRUG addiction, *ANIMAL models in research, *DRUG administration, SEX differences (Biology)

Abstract

Rationale: Consistent sex differences are observed in human drug addiction, with females often exceeding males on drug intake. However, there is still a need for animal models for some aspects of addiction such as acquisition of drug self-administration and the subsequent development of drug-seeking. Objectives: The present study examined sex differences in the acquisition and maintenance of self-administration of two widely used stimulants, cocaine and nicotine. Methods: Male and female rats self-administered cocaine (0.4 mg/kg/infusion) or nicotine (0.03 mg/kg/infusion) daily under a fixed-ratio 1 (FR 1) schedule until acquisition criteria were met (maximum of 30 sessions). The self-administration criterion for cocaine was ≥20 infusions in a 2-h session and ≥5 infusions in a 1-h session for nicotine. Sex differences were assessed by examining the percentage of rats that met acquisition criteria, the number of sessions to meet criteria, and the number of infusions earned during the maintenance phase. Results: A significantly higher percentage of male rats acquired both cocaine and nicotine self-administration than females, and males met acquisition criteria in fewer sessions. However, after criteria were met, females self-administered more cocaine than males during the first 5 days of maintenance. There were no sex differences in nicotine infusions post-acquisition. Conclusions: Differences in acquisition amongst sexes can reveal factors that are integral to initiation of drug use, an often overlooked phase of drug addiction. [ABSTRACT FROM AUTHOR]

Published

2016

49. Social dominance in rats: effects on cocaine self-administration, novelty reactivity and dopamine receptor binding and content in the striatum.

Author

Jupp, Bianca, Murray, Jennifer, Jordan, Emily, Xia, Jing, Fluharty, Meg, Shrestha, Saurav, Robbins, Trevor, and Dalley, Jeffrey

Subjects

*SOCIAL dominance, *COCAINE, *DOPAMINE receptors, *DRUG administration, *SOCIAL status, *DRUG addiction, *TASK performance, *LABORATORY rats

Abstract

Rationale: Studies in human and non-human primates demonstrate that social status is an important determinant of cocaine reinforcement. However, it is unclear whether social rank is associated with other traits that also predispose to addiction and whether social status similarly predicts cocaine self-administration in rats. Objectives: The objective of this study is to investigate whether social ranking assessed using a resource competition task affects (i) the acquisition, maintenance and reinstatement of cocaine self-administration; (ii) the dopaminergic markers in the striatum; and (iii) the expression of ancillary traits for addiction. Methods: Social ranking was determined in group-housed rats based upon drinking times during competition for a highly palatable liquid. Rats were then evaluated for cocaine self-administration and cue-induced drug reinstatement or individual levels of impulsivity, anxiety and novelty-induced locomotor activity. Finally, dopamine content, dopamine transporter (DAT) and dopamine D/D (D) receptor binding were measured postmortem in the dorsal and ventral striatum. Results: Rats deemed socially dominant showed enhanced novelty reactivity but were neither more impulsive nor anxious compared with subordinate rats. Dominant rats additionally maintained higher rates of cocaine self-administration but showed no differences in the acquisition, extinction and reinstatement of this behaviour. D binding was elevated in the nucleus accumbens shell and dorsal striatum of dominant rats when compared to subordinate rats, and was accompanied by elevated DAT and reduced dopamine content in the nucleus accumbens shell. Conclusions: These findings show that social hierarchy influences the rate of self-administered cocaine but not anxiety or impulsivity in rats. Similar to non-human primates, these effects may be mediated by striatal dopaminergic systems. [ABSTRACT FROM AUTHOR]

Published

2016

50. Ghrelin and endocannabinoids participation in morphine-induced effects in the rat nucleus accumbens.

Author

Sustkova-Fiserova, Magdalena, Jerabek, Pavel, Havlickova, Tereza, Syslova, Kamila, and Kacer, Petr

Subjects

*GHRELIN, *CANNABINOIDS, *ANANDAMIDE, *NUCLEUS accumbens, *DRUG addiction, *DOPAMINE, *OPIOIDS, *LABORATORY rats

Abstract

Rationale and objectives: In addition to dopamine, endocannabinoids are thought to participate in neural reward mechanisms of opioids. Number of recent studies suggests crucial involvement of ghrelin in some addictive drugs effects. Our previous results showed that ghrelin participates in morphine-induced changes in the mesolimbic dopaminergic system associated with reward processing. The goal of the present study was to test whether the growth hormone secretagogue receptor (GHS-R1A) antagonist JMV2959 was able to influence morphine-induced effects on anandamide (N-arachidonoylethanolamine, AEA) and 2-arachidonoylglycerol (2-AG) in the nucleus accumbens shell (NACSh). Methods: We used in vivo microdialysis to determine changes in levels of AEA and 2-AG in the NACSh in rats following (i) an acute morphine dose (5, 10 mg/kg s.c.) with and without JMV2959 pretreatment (3, 6 mg/kg i.p.) or (ii) a morphine challenge dose (5 mg/kg s.c.) with and without JMV2959 (3, 6 mg/kg i.p.) pretreatment, administered during abstinence following repeated doses of morphine (5 days, 10-40 mg/kg). Co-administration of ghrelin (40 ug/kg i.p.) was used to verify the ghrelin mechanisms involvement. Results: Pretreatment with JMV2959 significantly and dose-dependently reversed morphine-induced anandamide increases in the NACSh in both the acute and longer-term models, resulting in a significant AEA decrease. JMV2959 significantly intensified acute morphine-induced decreases in accumbens 2-AG levels and attenuated morphine challenge-induced 2-AG decreases. JMV2959 pretreatment significantly reduced concurrent morphine challenge-induced behavioral sensitization. JMV2959 pretreatment effects were abolished by co-administration of ghrelin. Conclusions: Our results indicate significant involvement of ghrelin signaling in morphine-induced endocannabinoid changes in the NACSh. [ABSTRACT FROM AUTHOR]

Published

2016