Your search keyword '"S. Stevens Negus"' showing total 481 results

1. Effects of Selective and Mixed-Action Kappa and Delta Opioid Receptor Agonists on Pain-Related Behavioral Depression in Mice

Author

S. Stevens Negus, Celsey M. St. Onge, Young K. Lee, Mengchu Li, Kenner C. Rice, and Yan Zhang

Subjects

kappa opioid receptor, delta opioid receptor, nalfurafine, SNC80, hydrocodone, aprepitant, Organic chemistry, QD241-441

Abstract

We recently developed a series of nalfurafine analogs (TK10, TK33, and TK35) that may serve as non-addictive candidate analgesics. These compounds are mixed-action agonists at the kappa and delta opioid receptors (KOR and DOR, respectively) and produce antinociception in a mouse warm-water tail-immersion test while failing to produce typical mu opioid receptor (MOR)-mediated side effects. The warm-water tail-immersion test is an assay of pain-stimulated behavior vulnerable to false-positive analgesic-like effects by drugs that produce motor impairment. Accordingly, this study evaluated TK10, TK33, and TK35 in a recently validated assay of pain-related behavioral depression in mice that are less vulnerable to false-positive effects. For comparison, we also evaluated the effects of the MOR agonist/analgesic hydrocodone (positive control), the neurokinin 1 receptor (NK1R) antagonist aprepitant (negative control), nalfurafine as a selective KOR agonist, SNC80 as a selective DOR agonist, and a nalfurafine/SNC80 mixture. Intraperitoneal injection of dilute lactic acid (IP lactic acid) served as a noxious stimulus to depress vertical and horizontal locomotor activity in male and female ICR mice. IP lactic acid-induced locomotor depression was alleviated by hydrocodone but not by aprepitant, nalfurafine, SNC80, the nalfurafine/SNC80 mixture, or the KOR/DOR agonists. These results suggest that caution is warranted in advancing mixed-action KOR/DOR agonists as candidate analgesics.

Published

2024

2. Role of mu opioid receptor (MOR) agonist efficacy as a determinant of opioid antinociception in a novel assay of pain-depressed behavior in female and male mice

Author

S. Stevens Negus, Hamid I. Akbarali, Minho Kang, Young K. Lee, Samuel A. Marsh, Edna J. Santos, and Yan Zhang

Subjects

efficacy, analgesia, pain-depressed behavior, mice, locomotor, mu opioid agonist, Neurology. Diseases of the nervous system, RC346-429

Abstract

IntroductionIntermediate efficacy mu opioid receptor (MOR) agonists have potential to retain analgesic effectiveness while improving safety, but the optimal MOR efficacy for effective and safe opioid analgesia is unknown. Preclinical assays of pain-depressed behavior can assess effects of opioids and other candidate analgesics on pain-related behavioral depression, which is a common manifestation of clinically relevant pain and target of pain treatment. Accordingly, the present study goal was to validate a novel assay of pain-depressed locomotor behavior in mice and evaluate the role of MOR efficacy as a determinant of opioid analgesic effects and related safety measures.MethodsMale and female ICR mice were tested in a locomotor chamber consisting of 2 compartments connected by a doorway that contained a 1-inch-tall barrier. Dependent measures during 15-min behavioral sessions included crosses between compartments (which required vertical activity to surmount the barrier) and total movement counts (which required horizontal activity to break photobeams in each compartment).Results and DiscussionIntraperitoneal injection of lactic acid (IP acid) produced a concentration- and time-dependent depression of both endpoints. Optimal blockade of IP acid-induced behavioral depression with minimal motor impairment was achieved with intermediate-efficacy MOR treatments that also produced less gastrointestinal-transit inhibition and respiratory depression than the high-efficacy MOR agonist fentanyl. Sex differences in treatment effects were rare. Overall, these findings validate a novel procedure for evaluating opioids and other candidate analgesic effects on pain-related behavioral depression in mice and support continued research with intermediate-efficacy MOR agonists as a strategy to retain opioid analgesic effectiveness with improved safety.

Published

2023

3. Role of efficacy as a determinant of locomotor activation by mu‐opioid receptor (MOR) ligands in female and male mice. II. Effects of novel MOR‐selective phenylmorphans with high‐to‐low MOR efficacy

Author

Edna J. Santos, Nima Nassehi, Eric W. Bow, Dana R. Chambers, Eugene S. Gutman, Arthur E. Jacobson, Joshua A. Lutz, Samuel A. Marsh, Kenner C. Rice, Agnieszka Sulima, Dana E. Selley, and S. Stevens Negus

Subjects

efficacy, mouse, mu opioid receptor, opioid, locomotor activity, receptor binding, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Low‐efficacy mu‐opioid receptor (MOR) agonists represent promising therapeutics, but existing compounds (e.g., buprenorphine, nalbuphine) span a limited range of low MOR efficacies and have poor MOR selectivity. Accordingly, new and selective low‐efficacy MOR agonists are of interest. A novel set of chiral C9‐substituted phenylmorphans has been reported to display improved MOR selectivity and a range of high‐to‐low MOR efficacies under other conditions; however, a full opioid receptor binding profile for these drugs has not been described. Additionally, studies in mice will be useful for preclinical characterization of these novel compounds, but the pharmacology of these drugs in mice has also not been examined. Accordingly, the present study characterized the binding selectivity and in vitro efficacy of these compounds using assays of opioid receptor binding and ligand‐stimulated [35S]GTPɣS binding. Additionally, locomotor effects were evaluated as a first step for in vivo behavioral assessment in mice. The high‐efficacy MOR agonist and clinically effective antidepressant tianeptine was included as a comparator. In binding studies, all phenylmorphans showed improved MOR selectivity relative to existing lower‐efficacy MOR agonists. In the ligand‐stimulated [35S]GTPɣS binding assay, seven phenylmorphans had graded levels of sub‐buprenorphine MOR efficacy. In locomotor studies, the compounds again showed graded efficacy with a rapid onset and ≥1 h duration of effects, evidence for MOR mediation, and minor sex differences. Tianeptine functioned as a high‐efficacy MOR agonist. Overall, these in vitro and in vivo studies support the characterization of these compounds as MOR‐selective ligands with graded MOR efficacy and utility for further behavioral studies in mice.

Published

2023

4. Climbing behavior by mice as an endpoint for preclinical assessment of drug effects in the absence and presence of pain

Author

Edna J. Santos, Arianna N. Giddings, Farah A. Kandil, and S. Stevens Negus

Subjects

pain, ICR mice, climbing, opioids, efficacy, Neurology. Diseases of the nervous system, RC346-429

Abstract

This study evaluated climbing in mice as a tool to assess the expression and treatment of pain-related behavioral depression in male and female ICR mice. Mice were videotaped during 10-min sessions in a vertical plexiglass cylinder with wire mesh walls, and “Time Climbing” was scored by observers blind to treatments. Initial validation studies demonstrated that baseline climbing was stable across repeated days of testing and depressed by intraperitoneal injection of dilute lactic acid (IP acid) as an acute pain stimulus. Additionally, IP acid-induced depression of climbing was blocked by the positive-control non-steroidal anti-inflammatory drug (NSAID) ketoprofen but not by the negative control kappa opioid receptor agonist U69593. Subsequent studies examined effects of single-molecule opioids (fentanyl, buprenorphine, naltrexone) and of fixed-proportion fentanyl/naltrexone mixtures (10:1, 3.2:1, and 1:1) that vary in their efficacy at the mu opioid receptor (MOR). Opioids administered alone produced a dose- and efficacy-dependent decrease in climbing, and fentanyl/naltrexone-mixture data indicated that climbing in mice is especially sensitive to disruption by even low-efficacy MOR activation. Opioids administered as a pretreatment to IP acid failed to block IP acid-induced depression of climbing. Taken together, these findings support the utility of climbing in mice as an endpoint to evaluate candidate-analgesic effectiveness both to (a) produce undesirable behavioral disruption when the test drug is administered alone, and (b) produce a therapeutic blockade of pain-related behavioral depression. The failure of MOR agonists to block IP acid-induced depression of climbing likely reflects the high sensitivity of climbing to disruption by MOR agonists.

Published

2023

5. Editorial: Preclinical Animal Models and Measures of Pain: Improving Predictive Validity for Analgesic Drug Development

Author

Anke Tappe-Theodor, S. Stevens Negus, and Thomas J. Martin

Subjects

pain, animal model, analgesics, drug development, inflammation, neuropathic, Neurology. Diseases of the nervous system, RC346-429

Published

2022

6. Morphine Exacerbates Experimental Colitis-Induced Depression of Nesting in Mice

Author

Stanley M. Cheatham, Karan H. Muchhala, Eda Koseli, Joanna C. Jacob, Essie Komla, S. Stevens Negus, and Hamid I. Akbarali

Subjects

opioids, depression, inflammation, analgesia, tolerance, colitis, Neurology. Diseases of the nervous system, RC346-429

Abstract

Opioids and non-steroidal anti-inflammatory drugs (NSAIDs) are excellent analgesics, but recent clinical evidence suggests that these drugs might worsen disease severity in Crohn's disease patients, limiting their clinical utility for treating Inflammatory Bowel Disease (IBD). One indicator of change in well-being from conditions such as IBD is behavioral depression and disruption to activities of daily living. Preclinical measures of behavioral depression can provide an indicator of changes in quality of life and subsequent modification by candidate analgesics. In mice, nesting is an adaptive unconditioned behavior that is susceptible to disruption by noxious stimuli, and some types of pain related nesting depression are responsive to opioid and NSAID analgesics. Here we show that a 2, 4, 6-trinitrobenzene sulfonic acid (TNBS) model of experimental colitis depresses nesting behavior in mice, and we evaluated effects of morphine, an opioid, and ketoprofen, a NSAID, on TNBS-induced nesting depression. In Swiss Webster mice, TNBS significantly reduced nesting that peaked on Day 3 and recovered in a time-dependent manner with complete recovery by Day 7. In the absence of colonic inflammation, daily treatment with morphine (1–10 mg/kg) did not decrease nesting except at 10mg/kg/day. However, in TNBS-treated mice 3.2 mg/kg/day morphine significantly exacerbated TNBS-induced nesting depression and delayed recovery. While 3.2 mg/kg/day morphine alone did not alter locomotor activity and TNBS-induced depression of locomotion recovered, the combination of TNBS and 3.2 mg/kg/day morphine significantly attenuated locomotion and prevented recovery. Daily treatment with 3.2 or 10 mg/kg ketoprofen in TNBS-treated mice did not prevent depression of nesting. These data suggest that opioid analgesics but not NSAIDS worsen colonic inflammation-induced behavioral depression. Furthermore, these findings highlight the importance of evaluating analgesic effects in models of colonic inflammation induced depression of behavior.

Published

2021

7. Resistance of Food-Maintained Operant Responding to Mechanical Punishment in Rats: Further Evidence for Weak 'Affective/Motivational Pain' in Rat Models of Inflammatory and Neuropathic Pain

Author

S. Stevens Negus, S. A. Marsh, and E. A. Townsend

Subjects

complete freund adjuvant, paclitaxel, Operant, punishment, naltrexone, U69,593, Therapeutics. Pharmacology, RM1-950

Abstract

Clinically relevant chronic pain is often associated with functional impairment and behavioral depression as an “affective/motivational” sign of pain; however preclinical animal models of inflammatory and neuropathic pain often produce weak evidence of impaired function. We hypothesized that hindpaw mechanical stimulation produced by a requirement to rear on a textured “NOX” plate would punish operant responding in rats treated with intraplantar complete Freund’s adjuvant (CFA, a model of inflammatory pain) or the chemotherapeutic paclitaxel (PTX, a model of neuropathic pain) and produce sustained pain-related depression of operant behavior. Male Sprague–Dawley rats were trained under a progressive-ratio (PR) schedule of food-maintained operant responding, then treated with CFA (100 µL in left hindpaw), PTX (2.0 mg/kg IP on alternate days for four total injections; 6.6 mg/kg IV on alternate days for three total injections), or saline vehicle. PR break points and mechanical thresholds for paw withdrawal from von Frey filaments were then tracked for 28 days. Subsequently, rats were tested with the opioid receptor antagonist naltrexone to assess latent sensitization and with the kappa opioid receptor (KOR) agonist U69593 to assess KOR function. CFA produced significant mechanical hypersensitivity for 3 weeks but decreased PR breakpoints for only 1 day. Both IP and IV PTX produced mechanical hypersensitivity for at least three weeks; however, only IV PTX decreased PR breakpoints, and this decrease was not alleviated by morphine. After recovery, naltrexone reinstated mechanical hypersensitivity in CFA- but not PTX-treated rats, and it did not reinstate depression of breakpoints in any group. U69593 dose-dependently decreased PR breakpoints in all groups with no difference between control vs. CFA/PTX groups. These results suggest that rearing on a textured NOX plate was not sufficient to punish operant responding in CFA- and PTX-treated rats despite the presence of sustained mechanical hypersensitivity. The rapid recovery of operant responding could not be attributed to latent sensitization, KOR downregulation, or behavioral tolerance. These results extend the range of conditions under which putative chronic pain manipulations produce weak evidence for depression of operant responding as a sign of the “affective/motivational” component of pain in rats.

Published

2021

8. A strategy to prioritize emerging drugs of abuse for analysis: Abuse liability testing using intracranial self-stimulation (ICSS) in rats and validation with α-pyrrolidinohexanophenone (α-PHP)

Author

Tyson R. Baird, Rachel A. Davies, Richard A. Glennon, Michelle R. Peace, and S. Stevens Negus

Subjects

Novel psychoactive substances, Intracranial self-stimulation, Abuse liability testing, Synthetic cathinones, α-pyrrolidinohexanophenone, Pharmacy and materia medica, RS1-441

Abstract

Novel psychoactive substances (NPS) threaten public health and safety while also straining the limited resources of forensic laboratories. To efficiently allocate the finite resources available, we propose a new strategy for prioritizing NPS with abuse liability testing using a preclinical behavioral procedure in rats known as intracranial self-stimulation (ICSS). To validate this assay, the recently-scheduled synthetic cathinone α-PHP was compared to cocaine, a mechanistically similar drug of abuse, as a positive control and saline as a negative control. Male Sprague-Dawley rats (n=6) were implanted with electrodes targeting the medial forebrain bundle and trained to respond by lever-press for electrical brain stimulation. The rats were tested with doses of 0.32, 1.0, and 3.2 mg/kg α-PHP as well as 10 mg/kg of cocaine and saline administered by intraperitoneal injection. Neither saline nor 0.32 mg/kg α-PHP altered ICSS response rates compared to baseline levels of responding; however, doses of 1.0 and 3.2 mg/kg α-PHP and 10 mg/kg cocaine facilitated ICSS responding. This ICSS profile suggests that α-PHP has high abuse potential, with a rapid onset of effects and a long duration of action, and supports the decision to schedule this compound. This study demonstrates the ability of ICSS to distinguish between compounds of low and high potential for abuse. A strategy is proposed here to screen NPS using ICSS and classify emerging drugs into four priority categories for further analysis.

Published

2021

9. Preclinical Determinants of Drug Choice under Concurrent Schedules of Drug Self-Administration

Author

Matthew L. Banks and S. Stevens Negus

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Drug self-administration procedures have played a critical role in the experimental analysis of psychoactive compounds, such as cocaine, for over 50 years. While there are numerous permutations of this procedure, this paper will specifically focus on choice procedures using concurrent schedules of intravenous drug self-administration. The aims of this paper are to first highlight the evolution of drug choice procedures and then review the subsequent preclinical body of literature utilizing these choice procedures to understand the environmental, pharmacological, and biological determinants of the reinforcing stimulus effects of drugs. A main rationale for this paper is our proposition that choice schedules are underutilized in investigating the reinforcing effects of drugs in assays of drug self-administration. Moreover, we will conclude with potential future directions and unexplored scientific space for the use of drug choice procedures.

Published

2012

10. Rate of onset of dopamine transporter inhibitors assessed with intracranial self-stimulation and in vivo dopamine photometry in rats

Author

Tyson R. Baird, Kimberly N. Karin, Samuel A. Marsh, F. Ivy Carroll, J. M. L. Medina-Contreras, S. Stevens Negus, and Jose M. Eltit

Subjects

Pharmacology

Published

2023

11. Effects of naltrexone on amphetamine choice in rhesus monkeys and rats

Author

Hannah L. Robinson, Megan Jo Moerke, Matthew L. Banks, and S. Stevens Negus

Subjects

Pharmacology, Psychiatry and Mental health, Pharmacology (medical)

Published

2023

12. Role of Efficacy as a Determinant of Locomotor Activation by Mu Opioid Receptor Ligands in Female and Male Mice

Author

Edna J. Santos, Matthew L. Banks, and S. Stevens Negus

Subjects

Male, Pharmacology, Dose-Response Relationship, Drug, Receptors, Opioid, mu, CHO Cells, Ligands, Naltrexone, Rats, Analgesics, Opioid, Fentanyl, Mice, Cricetulus, Behavioral Pharmacology, Cricetinae, Animals, Molecular Medicine, Female

Abstract

Mu opioid receptor (MOR) agonists produce locomotor hyperactivity in mice as one sign of opioid-induced motor disruption. The goal of this study was to evaluate the degree of MOR efficacy required to produce this hyperactivity. Full dose-effect curves were determined for locomotor activation produced in male and female Institute of Cancer Research (ICR) mice by (1) eight different single-molecule opioids with high to low MOR efficacy and (2) a series of fixed-proportion fentanyl/naltrexone mixtures with high to low fentanyl proportions. Data from the mixtures were used to quantify the efficacy requirement for MOR agonist-induced hyperactivity relative to efficacy requirements determined previously for other MOR agonist effects. Specifically, efficacy requirement was quantified as the EP50 value, which is the “Effective Proportion” of fentanyl in a fentanyl/naltrexone mixture that produces a maximal effect equal to 50% of the maximal effect of fentanyl alone. Maximal hyperactivity produced by each drug and mixture in the present study correlated with previously published data for maximal stimulation of GTPɣS binding in MOR-expressing Chinese hamster ovary cells as an in vitro measure of relative efficacy. Additionally, the EP(50) value for hyperactivity induced by fentanyl/naltrexone mixtures indicated that opioid-induced hyperactivity in mice has a relatively high efficacy requirement in comparison with some other MOR agonist effects, and in particular is higher than the efficacy requirement for thermal antinociception in mice or fentanyl discrimination in rats. Taken together, these data show that MOR agonist-induced hyperactivity in mice is efficacy dependent and requires relatively high levels of MOR agonist efficacy for its full expression. SIGNIFICANCE STATEMENT: Mu opioid receptor (MOR) agonist-induced hyperlocomotion in mice is dependent on the MOR efficacy of the agonist and requires a relatively high degree of efficacy for its full expression.

Published

2022

13. Effects of the 5-HT2A receptor antagonist volinanserin on head-twitch response and intracranial self-stimulation depression induced by different structural classes of psychedelics in rodents

Author

Alaina M. Jaster, Harrison Elder, Samuel A. Marsh, Mario de la Fuente Revenga, S. Stevens Negus, and Javier González-Maeso

Subjects

Pharmacology

Published

2022

14. Characterization of a Potential KOR/DOR Dual Agonist with No Apparent Abuse Liability via a Complementary Structure-Activity Relationship Study on Nalfurafine Analogues

Author

Mengchu Li, David L. Stevens, Michelle Arriaga, E. Andrew Townsend, Rolando E. Mendez, Nadejda A. Blajkevch, Dana E. Selley, Matthew L. Banks, S. Stevens Negus, William L. Dewey, and Yan Zhang

Subjects

Physiology, Cognitive Neuroscience, Cell Biology, General Medicine, Biochemistry, Article

Abstract

Discovery of analgesics void of abuse liability is critical to battle the opioid crisis in the United States. Among many strategies to achieve this goal, targeting more than one opioid receptor seems promising to minimize this unwanted side effect while achieving a reasonable therapeutic profile. In the process of understanding the structure-activity relationship of nalfurafine, we identified a potential analgesic agent, NMF, as a dual kappa opioid receptor/delta opioid receptor agonist with minimum abuse liability. Further characterizations, including primary in vitro ADMET studies (hERG toxicity, plasma protein binding, permeability, and hepatic metabolism), and in vivo pharmacodynamic and toxicity profiling (time course, abuse liability, tolerance, withdrawal, respiratory depression, body weight, and locomotor activity) further confirmed NMF as a promising drug candidate for future development.

Published

2022

15. Effects of environmental manipulations on cocaine-vs-social choice in male and female rats

Author

Madison M. Marcus, S. Stevens Negus, and Matthew L. Banks

Subjects

Pharmacology, Male, Reinforcement Schedule, Dose-Response Relationship, Drug, Clinical Biochemistry, Self Administration, Toxicology, Biochemistry, Choice Behavior, Article, Rats, Behavioral Neuroscience, Cocaine, Animals, Conditioning, Operant, Female, Biological Psychiatry

Abstract

Cocaine use disorder occurs in an environment where cocaine and other nondrug commodities are concurrently available. Preclinical drug-vs-nondrug choice procedures are one simplified method of modeling this complex clinical environment. The present study established a discrete-trial progressive-ratio (PR) cocaine-vs-social interaction choice procedure in male and female rats and determined sensitivity of choice behavior to manipulations of reinforcer magnitude and non-contingent “sample” reinforcer presentation. Rats could make up to nine discrete choices between an intravenous cocaine infusion (0.1 – 1.0 mg/kg/inf) and social interaction with a same-sex social “Partner” rat. Cocaine infusions were available under a PR schedule of reinforcement, and social interaction was available under a fixed-ratio (FR) 3 schedule. Social interaction was chosen over no or small cocaine doses (saline, 0.01 mg/kg/inf) and behavior was reallocated away from social and towards cocaine at larger cocaine doses (1.0 mg/kg/inf). Manipulating social interaction time as one method to alter social reinforcer magnitude did not significantly alter cocaine-vs-social choice. Removing the non-contingent reinforcer presentations before the discrete choice trials also failed to affect cocaine-vs-social choice, suggesting the time interval was sufficient to minimize any potential influence of the non-contingent cocaine infusions on subsequent choice behavior. Overall, the present results were consistent with previous drug-vs-social choice studies and extend our knowledge of environmental factors impacting drug-vs-social choice. Future studies determining the pharmacological sensitivity of cocaine-vs-social choice will be important in expanding the preclinical utility of these procedures for candidate medication drug development.

Published

2022

16. Behavioral Battery for Testing Candidate Analgesics in Mice. II. Effects of Endocannabinoid Catabolic Enzyme Inhibitors and ∆9-Tetrahydrocannabinol

Author

Clare M Diester, S. Stevens Negus, and Aron H. Lichtman

Subjects

Male, Nociception, 0301 basic medicine, medicine.medical_treatment, Intraperitoneal injection, Drug Evaluation, Preclinical, Pharmacology, Amidohydrolases, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Rimonabant, Fatty acid amide hydrolase, Noxious stimulus, medicine, Animals, Dronabinol, Enzyme Inhibitors, Tetrahydrocannabinol, Analgesics, Mice, Inbred ICR, Fatty acid amide, Behavior, Animal, Endocannabinoid system, Monoacylglycerol Lipases, Monoacylglycerol lipase, 030104 developmental biology, chemistry, Behavioral Pharmacology, Molecular Medicine, Female, 030217 neurology & neurosurgery, medicine.drug

Abstract

Enhanced signaling of the endocannabinoid (eCB) system through inhibition of the catabolic enzymes monoacylglycerol lipase (MAGL) and fatty acid amide hydrolase (FAAH) has received increasing interest for development of candidate analgesics. This study compared effects of MAGL and FAAH inhibitors with effects of ∆9-tetrahydrocannabinol (THC) using a battery of pain-stimulated, pain-depressed, and pain-independent behaviors in male and female mice. Intraperitoneal injection of dilute lactic acid (IP acid) served as an acute visceral noxious stimulus to stimulate two behaviors (stretching, facial grimace) and depress two behaviors (rearing, nesting). Nesting and locomotion were also assessed in the absence of IP acid as pain-independent behaviors. THC and a spectrum of six eCB catabolic enzyme inhibitors ranging from MAGL- to FAAH-selective were assessed for effectiveness to alleviate pain-related behaviors at doses that did not alter pain-independent behaviors. The MAGL-selective inhibitor MJN110 produced the most effective antinociceptive profile, with 1.0 mg/kg alleviating IP acid effects on stretching, grimace, and nesting without altering pain-independent behaviors. MJN110 effects on IP acid-depressed nesting had a slow onset and long duration (40 minutes to 6 hours), were blocked by rimonabant, and tended to be greater in females. As inhibitors increased in FAAH selectivity, antinociceptive effectiveness decreased. PF3845, the most FAAH-selective inhibitor, produced no antinociception up to doses that disrupted locomotion. THC decreased IP acid-stimulated stretching and grimace at doses that did not alter pain-independent behaviors; however, it did not alleviate IP acid-induced depression of rearing or nesting. These results support further consideration of MAGL-selective inhibitors as candidate analgesics for acute inflammatory pain. SIGNIFICANCE STATEMENT: This study characterized a spectrum of endocannabinoid catabolic enzyme inhibitors ranging in selectivity from monoacylglycerol lipase-selective to fatty acid amide hydrolase-selective in a battery of pain-stimulated, pain-depressed, and pain-independent behaviors previously pharmacologically characterized in a companion paper. This battery provides a method for prioritizing candidate analgesics by effectiveness to alleviate pain-related behaviors at doses that do not alter pain-independent behaviors, with inclusion of pain-depressed behaviors increasing translational validity and decreasing susceptibility to motor-depressant false positives.

Published

2021

17. Effect of TRV130 and methadone on fentanyl-vs.-food choice and somatic withdrawal signs in opioid-dependent and post-opioid-dependent rats

Author

E. Andrew Townsend, Bruce E. Blough, David H. Epstein, S. Stevens Negus, Yavin Shaham, and Matthew L. Banks

Subjects

Pharmacology, Male, Narcotics, Thiophenes, Opioid-Related Disorders, Buprenorphine, Rats, Substance Withdrawal Syndrome, Analgesics, Opioid, Fentanyl, Psychiatry and Mental health, Receptors, Opioid, Animals, Spiro Compounds, Methadone

Abstract

The high efficacy mu-opioid receptor (MOR) agonist methadone is an effective opioid use disorder (OUD) medication used exclusively in opioid-dependent patients. However, methadone has undesirable effects that limit its clinical efficacy. Intermediate efficacy MOR agonists may treat OUD with fewer undesirable effects. We compared the effects of methadone with the intermediate efficacy MOR agonist TRV130 (oliceridine) on fentanyl-vs.-food choice and somatic withdrawal signs in opioid-dependent and post-opioid-dependent rats. Male rats (n = 20) were trained under a fentanyl-vs.-food choice procedure. Rats were then provided extended fentanyl (3.2 µg/kg/infusion) access (6 p.m.-6 a.m.) for 10 days to produce opioid dependence/withdrawal. Rats were treated with vehicle (n = 7), TRV130 (3.2 mg/kg; n = 8), or methadone (3.2 mg/kg; n = 5) three times per day after each extended-access session (8:30 a.m., 11 a.m., 1:30 p.m.). Withdrawal sign scoring (1:55 p.m.) and choice tests (2-4 p.m.) were conducted daily. Vehicle, TRV130, and methadone effects on fentanyl choice were redetermined in post-opioid-dependent rats. Vehicle-, TRV130-, and methadone-treated rats had similar fentanyl intakes during extended access. Vehicle-treated rats exhibited increased withdrawal signs and decreased bodyweights. Both methadone and TRV130 decreased these withdrawal signs. TRV130 was less effective than methadone to decrease fentanyl choice and increase food choice in opioid-dependent rats. Neither methadone nor TRV130 decreased fentanyl choice in post-opioid-dependent rats. Results suggest that higher MOR activation is required to reduce fentanyl choice than withdrawal signs in fentanyl-dependent rats. Additionally, given that TRV130 did not precipitate withdrawal in opioid-dependent rats, intermediate efficacy MOR agonists like TRV130 may facilitate the transition of patients with OUD from methadone to lower efficacy treatments like buprenorphine.

Published

2022

18. In a Rat Model of Opioid Maintenance, the G Protein–Biased Mu Opioid Receptor Agonist TRV130 Decreases Relapse to Oxycodone Seeking and Taking and Prevents Oxycodone-Induced Brain Hypoxia

Author

Shruthi A. Thomas, Bruce E. Blough, David Perekopskiy, David H. Epstein, Eugene A. Kiyatkin, Jennifer K. Hoots, Ida Fredriksson, Anum Afzal, Yavin Shaham, Hannah Korah, S. Stevens Negus, and Jennifer M. Bossert

Subjects

0301 basic medicine, Agonist, medicine.drug_class, business.industry, Context (language use), Pharmacology, Relapse prevention, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Opioid, medicine, μ-opioid receptor, business, Oxycodone, 030217 neurology & neurosurgery, Biological Psychiatry, Methadone, medicine.drug, Buprenorphine

Abstract

Background Maintenance treatment with opioid agonists (buprenorphine, methadone) is effective for opioid addiction but does not eliminate opioid use in all patients. We modeled maintenance treatment in rats that self-administered the prescription opioid oxycodone. The maintenance medication was either buprenorphine or the G protein–biased mu opioid receptor agonist TRV130. We then tested prevention of oxycodone seeking and taking during abstinence using a modified context-induced reinstatement procedure, a rat relapse model. Methods We trained rats to self-administer oxycodone (6 hours/day, 14 days) in context A; infusions were paired with discrete tone-light cues. We then implanted osmotic pumps containing buprenorphine or TRV130 (0, 3, 6, or 9 mg/kg/day) and performed 3 consecutive tests: lever pressing reinforced by oxycodone-associated discrete cues in nondrug context B (extinction responding), context-induced reinstatement of oxycodone seeking in context A, and reacquisition of oxycodone self-administration in context A. We also tested whether TRV130 maintenance would protect against acute oxycodone-induced decreases in nucleus accumbens oxygen levels. Results In male rats, buprenorphine and TRV130 decreased extinction responding and reacquisition of oxycodone self-administration but had a weaker (nonsignificant) effect on context-induced reinstatement. In female rats, buprenorphine decreased responding in all 3 tests, while TRV130 decreased only extinction responding. In both sexes, TRV130 prevented acute brain hypoxia induced by moderate doses of oxycodone. Conclusions TRV130 decreased oxycodone seeking and taking during abstinence in a partly sex-specific manner and prevented acute oxycodone-induced brain hypoxia. We propose that G protein–biased mu opioid receptor agonists, currently in development as analgesics, should be considered as relapse prevention maintenance treatment for opioid addiction.

Published

2020

19. Preclinical assessment of tramadol abuse potential: Effects of acute and repeated tramadol on intracranial self-stimulation in rats

Author

Ahmad A. Altarifi, Mohammad Alsalem, S. Stevens Negus, and Megan J. Moerke

Subjects

Pharmacology, 0303 health sciences, business.industry, Analgesic, Transporter, Stimulation, Norepinephrine (medication), 03 medical and health sciences, Psychiatry and Mental health, 0302 clinical medicine, Morphine, Medicine, Pharmacology (medical), Serotonin, Tramadol, business, Receptor, 030217 neurology & neurosurgery, 030304 developmental biology, medicine.drug

Abstract

Background: Tramadol is a widely used analgesic that activates mu-opioid receptors (MOR) and inhibits serotonin and norepinephrine transporters. This mixed pharmacology may limit both its own abuse potential and its modulation of abuse potential of other MOR agonists. Aims: This study used an intracranial self-stimulation (ICSS) procedure to compare abuse-related effects produced by acute or repeated treatment with tramadol or morphine in rats. Abuse potential in ICSS procedures is indicated by a drug-induced increase (or ‘facilitation’) of ICSS responding. Methods: Adult male Sprague–Dawley rats were implanted with electrodes targeting the medial forebrain bundle and trained to respond on a lever for pulses of electrical brain stimulation. Tramadol effects were evaluated after acute administration (3.2–32 mg/kg) in the absence or presence of the opioid antagonist naltrexone, the CYP2D6 hepatic-enzyme inhibitor quinine or a combination of both. Additionally, both tramadol and morphine were also tested before and after repeated tramadol (32 mg/kg/day for six days) or repeated morphine (3.2 mg/kg/day for six days). Results: Acute tramadol produced primarily ICSS rate-decreasing effects that were antagonised by naltrexone but not by quinine or naltrexone + quinine. Tramadol also produced little or no ICSS facilitation after repeated tramadol or repeated morphine, and repeated tramadol did not enhance ICSS facilitation by morphine. By contrast, morphine-induced ICSS facilitation was enhanced by repeated morphine treatment. Conclusions: These results suggest that tramadol has lower abuse potential than other abused MOR agonists and that repeated tramadol exposure produces relatively little enhancement of abuse potential of other MOR agonists.

Published

2020

20. Evaluation of a Dual Fentanyl/Heroin Vaccine on the Antinociceptive and Reinforcing Effects of a Fentanyl/Heroin Mixture in Male and Female Rats

Author

Paul T. Bremer, Hannah L. Robinson, S. Stevens Negus, Kaycee E. Faunce, Matthew L. Banks, Alaina M Jaster, Kim D. Janda, and E. Andrew Townsend

Subjects

Male, Physiology, Cognitive Neuroscience, Pharmacology, Biochemistry, Article, Naltrexone, Fentanyl, Heroin, 03 medical and health sciences, 0302 clinical medicine, mental disorders, medicine, Animals, Potency, 030304 developmental biology, Vaccines, 0303 health sciences, Dose-Response Relationship, Drug, business.industry, Opioid use disorder, Cell Biology, General Medicine, medicine.disease, Rats, Analgesics, Opioid, Vaccination, Opioid, Female, business, 030217 neurology & neurosurgery, Methadone, medicine.drug

Abstract

Opioid-targeted vaccines represent an emerging treatment strategy for opioid use disorder. To determine whether concurrent vaccination against two commonly abused opioids (fentanyl and heroin) would confer broader spectrum opioid coverage, the current study evaluated dual fentanyl/heroin conjugate vaccine effectiveness using a warm water tail-withdrawal and a fentanyl/heroin-vs-food choice procedure in male and female rats across a 105-day observation period. Vaccine administration generated titers of high-affinity antibodies to both fentanyl and heroin sufficient to decrease the antinociceptive potency of fentanyl (25-fold), heroin (4.6-fold), and a 1:27 fentanyl/heroin mixture (7.5-fold). Vaccination did not alter the antinociceptive potency of the structurally dissimilar opioid agonist methadone. For comparison, continuous treatment with a naltrexone dose (0.032 mg/kg/h) shown previously to produce clinically relevant plasma-naltrexone levels decreased the antinociceptive potency of fentanyl, heroin, and the 1:27 fentanyl/heroin mixture by approximately 20-fold. Naltrexone treatment also shifted the potency of 1:27 fentanyl/heroin mixture in a drug-vs-food choice self-administration procedure 4.3-fold. In contrast, vaccination did not attenuate 1:27 fentanyl/heroin mixture self-administration in the drug-vs-food choice procedure. These data demonstrate that a vaccine can simultaneously attenuate the thermal antinociceptive effects of two structurally dissimilar opioids. However, the vaccine did not attenuate fentanyl/heroin mixture self-administration, suggesting a greater magnitude of vaccine responsiveness is required to decrease opioid reinforcement relative to antinociception.

Published

2020

21. Acute Pain-Related Depression of Operant Responding Maintained by Social Interaction or Food in Male and Female Rats

Author

A. N. Baldwin, M. L. Banks, S. A. Marsh, E. A. Townsend, M. Venniro, Y. Shaham, and S. Stevens Negus

Subjects

Pharmacology, Analgesics, Opioid, Male, Rats, Sprague-Dawley, Dose-Response Relationship, Drug, Morphine, Social Interaction, Animals, Conditioning, Operant, Female, Acute Pain, Article, Rats

Abstract

RATIONALE: Clinically relevant pain is associated with functional impairment and behavioral depression, including depression of social behavior. Moreover, recovery of function is a major goal in pain treatment. We used a recently developed model of operant responding for social interaction in rats to evaluate the vulnerability of social behavior to an experimental pain manipulation and the sensitivity of pain-depressed social behavior to treatment with clinically effective analgesics. METHODS: Sprague-Dawley male and female rats were trained to lever press for social access to another rat, and responding was evaluated after treatment with (a) intraperitoneal injection of dilute lactic acid (IP acid; 0.18–5.6%) administered alone as a visceral noxious stimulus, (b) the mu-opioid receptor (MOR) agonist morphine (0.32–10 mg/kg) or nonsteroidal anti-inflammatory drug (NSAID) ketoprofen (10 mg/kg) administered alone, or (c) morphine or ketoprofen administered before IP acid. For comparison, the same treatments were evaluated in separate rats trained to lever press for food delivery. RESULTS: Both IP acid alone and morphine alone more potently decreased responding maintained by social interaction than by food, whereas ketoprofen did not affect responding for either reinforcer. In general, analgesics were most effective to rescue operant responding when relatively low IP acid concentrations produced significant but submaximal behavioral depression; however, morphine was not effective to rescue responding for social interaction. CONCLUSIONS: Operant responding maintained by social interaction was more sensitive to pain-related disruption and less responsive to opioid analgesic rescue than food-maintained operant responding. Social behavior may be especially vulnerable to depression by pain states.

Published

2022

22. Contextual extinction of drug-associated discriminative stimuli fails to attenuate drug-vs-food choice in rhesus monkeys

Author

Matthew L. Banks, Blake A. Hutsell, and S. Stevens Negus

Subjects

Drug, Male, medicine.medical_specialty, media_common.quotation_subject, Drug availability, Experimental and Cognitive Psychology, Audiology, Article, Behavioral Neuroscience, 03 medical and health sciences, 0302 clinical medicine, Discriminative model, Cocaine, Recurrence, Food choice, Medicine, Animals, 030212 general & internal medicine, media_common, Dose-Response Relationship, Drug, business.industry, Addiction, Extinction (psychology), Macaca mulatta, 3. Good health, Heroin, Regimen, Pharmaceutical Preparations, Female, business, 030217 neurology & neurosurgery, Cocaine abuse

Abstract

Background: In drug addiction, relapse can be triggered by cues that function as discriminative stimuli to signal contingencies of drug availability and promote drug-taking behavior. Extinction procedures can weaken the association between drug-associated cues and drug use and may reduce the probability of relapse. This study evaluated effects of a regimen of extinction training on cocaine self-administration maintained in rhesus monkeys under a cocaine-vs.-food choice procedure that has been used previously to evaluate effectiveness of other candidate treatments for cocaine abuse. Methods: Behavior was initially maintained under a concurrent schedule of food delivery (1-g food pellets; fixed-ratio 100 schedule) and cocaine injections (0-0.1 mg/kg/injection; fixed-ratio 10 schedule) during daily 2-h choice sessions in male rhesus monkeys (n=4). Subsequently, choice sessions were supplemented by daily 20-h extinction sessions for 14 consecutive days. During extinction sessions, cocaine-associated discriminative stimuli were presented, but responding did not produce cocaine injections. Cocaine continued to be available during choice sessions. Results: Prior to extinction, cocaine maintained a dose-dependent increase in cocaine vs. food choice. Responding during extinction sessions declined to low levels by the fifth day. Exposure to extinction sessions produced a more gradual but significant decline in cocaine choice and a complementary increase in food choice during choice sessions. Conclusions: These preclinical results support the effectiveness of extinguishing cocaine-associated discriminative stimuli as a non-pharmacological treatment strategy for reducing cocaine choice. Moreover, these results also support the construct validity of preclinical drug vs. food choice procedures as a tool for candidate treatment evaluation for cocaine addiction.

Published

2022

23. Animal Models to Evaluate Expression, Mechanisms, and Treatment of Pain

Author

S. Stevens Negus

Subjects

Expression (architecture), business.industry, Medicine, Bioinformatics, business

Published

2022

24. Effects of the 5-HT

Author

Alaina M, Jaster, Harrison, Elder, Samuel A, Marsh, Mario, de la Fuente Revenga, S Stevens, Negus, and Javier, González-Maeso

Subjects

Mescaline, Serotonin, Depression, Rodentia, Tryptamines, Article, Psilocybin, Rats, Fluorobenzenes, Lysergic Acid Diethylamide, Mice, Self Stimulation, Piperidines, Phenethylamines, Hallucinogens, Animals, Receptor, Serotonin, 5-HT2A

Abstract

BACKGROUND: Clinical studies suggest that psychedelics exert robust therapeutic benefits in a number of psychiatric conditions including substance use disorder. Preclinical studies focused on safety and efficacy of these compounds are necessary to determine the full range of psychedelics’ effects. OBJECTIVES: The present study explores the behavioral pharmacology of structurally-distinct psychedelics in paradigms associated with serotonin 2A receptor (5-HT(2A)R) activation and behavioral disruption in two rodent models. Utilizing the selective 5-HT(2A)R antagonist volinanserin, we aimed to provide further pharmacological assessment of psychedelic effects in rodents. METHODS: We compared volinanserin (0.0001–0.1 mg/kg) antagonism of the phenethylamine 1-(2,5-dimethoxy-4-iodophenyl)-2-aminopropane (DOI, 1.0 mg/kg) and the ergoline lysergic acid diethylamide (LSD, 0.32 mg/kg) in preclinical assays predictive of hallucinations (head-twitch response or HTR in mice) and behavioral disruption (intracranial self-stimulation or ICSS in rats). Volinanserin antagonism of the phenethylamine mescaline, the tryptamine psilocybin, and the κ-opioid receptor agonist salvinorin A was also evaluated in the rat ICSS assay. RESULTS: Volinanserin had similar potency, effectiveness, and time-course to attenuate DOI-induced HTR in mice and ICSS depression in rats. Volinanserin completely blocked LSD-induced HTR in mice, but not LSD-induced ICSS depression in rats. Volinanserin also reversed ICSS depression by mescaline, but it was only partially effective to reduce the effects of psilocybin, and it exacerbated ICSS depression by salvinorin A. CONCLUSION: Although hallucination-related HTR behavior induced by phenethylamine, ergoline and tryptamine psychedelics appears to be 5-HT(2A)R-mediated, the receptor(s) responsible for behavioral disruptive effects may differ among these three structural classes.

Published

2021

25. Some effects of putative G-protein biased mu-opioid receptor agonists in male rhesus monkeys

Author

Matthew L. Banks, S. Stevens Negus, Bruce E. Blough, Laura M. Bohn, and Jeremy C. Cornelissen

Subjects

Agonist, Male, G protein, medicine.drug_class, Oliceridine, Receptors, Opioid, mu, Pain, Thiophenes, Pharmacology, Article, chemistry.chemical_compound, GTP-Binding Proteins, Medicine, Potency, Animals, Spiro Compounds, Oximetry, Respiratory system, Receptor, Analgesics, Behavior, Animal, business.industry, Respiration, Hypoxia (medical), Opioid-Related Disorders, Macaca mulatta, Psychiatry and Mental health, Nociception, chemistry, Drug Evaluation, medicine.symptom, business

Abstract

G-protein-biased mu-opioid receptor (GPB-MOR) agonists are an emerging class of compounds being evaluated as candidate analgesics and agonist medications for opioid use disorder. Most of the basic pharmacology of GPB-MOR agonists has been conducted in rodents and much less is known how the basic behavioral pharmacology of these compounds translates to nonhuman primates. The present study determined the antinociceptive potency and time course of three putative GPB-MOR agonists: (+)-oliceridine (i.e. TRV130), SR14968, and SR17018 in male rhesus monkeys (n = 3). In addition, the respiratory effects of these compounds were also indirectly determined using a pulse oximeter to measure percent peripheral oxygen saturation (%SpO2). The largest intramuscular oliceridine dose (3.2 mg/kg) produced significant antinociception at 50°C, but not 54°C, and peak effects were between 10 and 30 min. Oliceridine also decreased SpO2 below the 90% threshold that would be clinically categorized as hypoxia in two out of three monkeys. The largest intramuscular SR14968 dose (0.32 mg/kg) produced 100% MPE at 50°C, but not 54°C, in two out of three monkeys, and peak effects were between 30 and 100 min. The largest intravenous SR17018 dose (1 mg/kg) produced 100% MPE at 50°C, but not 54°C, in the same two out of three monkeys, and peak effects were between 30 and 100 min. Solubility limitations for both SR14968 and SR17018 impaired our ability to determine in-vivo potency and effectiveness on antinociceptive and %SpO2 measures for these two compounds.

Published

2021

26. A Strategy to Prioritize Emerging Drugs of Abuse for Analysis: Abuse Liability Testing Using Intracranial Self-Stimulation (ICSS) in Rats and Validation with α-Pyrrolidinohexanophenone (α-PHP)

Author

Richard A. Glennon, Tyson R. Baird, S. Stevens Negus, Michelle R. Peace, and Rachel A. Davies

Subjects

Drug, Drugs of abuse, business.industry, media_common.quotation_subject, medicine.medical_treatment, Intraperitoneal injection, Stimulation, Pharmacology, Intracranial self-stimulation, Article, RS1-441, Pharmacy and materia medica, Novel psychoactive substances, Abuse liability, Medicine, α-pyrrolidinohexanophenone, Abuse liability testing, Synthetic cathinones, business, Medial forebrain bundle, Saline, Electrical brain stimulation, media_common

Abstract

Novel psychoactive substances (NPS) threaten public health and safety while also straining the limited resources of forensic laboratories. To efficiently allocate the finite resources available, we propose a new strategy for prioritizing NPS with abuse liability testing using a preclinical behavioral procedure in rats known as intracranial self-stimulation (ICSS). To validate this assay, the recently-scheduled synthetic cathinone α-PHP was compared to cocaine, a mechanistically similar drug of abuse, as a positive control and saline as a negative control. Male Sprague-Dawley rats (n=6) were implanted with electrodes targeting the medial forebrain bundle and trained to respond by lever-press for electrical brain stimulation. The rats were tested with doses of 0.32, 1.0, and 3.2 mg/kg α-PHP as well as 10 mg/kg of cocaine and saline administered by intraperitoneal injection. Neither saline nor 0.32 mg/kg α-PHP altered ICSS response rates compared to baseline levels of responding; however, doses of 1.0 and 3.2 mg/kg α-PHP and 10 mg/kg cocaine facilitated ICSS responding. This ICSS profile suggests that α-PHP has high abuse potential, with a rapid onset of effects and a long duration of action, and supports the decision to schedule this compound. This study demonstrates the ability of ICSS to distinguish between compounds of low and high potential for abuse. A strategy is proposed here to screen NPS using ICSS and classify emerging drugs into four priority categories for further analysis.

Published

2021

27. Effectiveness comparisons of G-protein biased and unbiased mu opioid receptor ligands in warm water tail-withdrawal and drug discrimination in male and female rats

Author

Kathryn L. Schwienteck, Travis W. Grim, Bruce E. Blough, S. Stevens Negus, Samuel Obeng, Kaycee E. Faunce, Matthew L. Banks, Yan Zhang, and Kenner C. Rice

Subjects

Male, Nociception, Pain Threshold, 0301 basic medicine, Narcotic Antagonists, Receptors, Opioid, mu, Thiophenes, Pharmacology, Article, Naltrexone, Fentanyl, Discrimination Learning, Rats, Sprague-Dawley, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, medicine, Animals, Spiro Compounds, Morphine, Chemistry, Nalbuphine, Rats, Analgesics, Opioid, 030104 developmental biology, Opioid, Female, μ-opioid receptor, 030217 neurology & neurosurgery, medicine.drug, Buprenorphine, Methadone

Abstract

One emerging strategy to address the opioid crisis is the development of mu opioid receptor (MOR) ligands that preferentially signal the G-protein vs. β-arrestin pathway. The present study compared the relative potency and effectiveness of two G-protein biased (GPB)-MOR ligands TRV130 and SR-14968 to five unbiased MOR ligands (NAQ, nalbuphine, buprenorphine, morphine, and methadone) on therapeutic-related (e.g. antinociception) and abuse-related (e.g. discriminative stimulus effects) endpoints. Male and female rats were tested in a warm water tail-withdrawal procedure (50 °C) or trained to discriminate fentanyl (0.04 mg/kg, SC) from saline in a two-lever food-reinforced discrimination procedure. TRV130 and SR-14968 were approximately two-fold more potent to produce fentanyl stimulus effects vs. antinociception. Morphine, fentanyl, and methadone were significantly more potent in the fentanyl discrimination vs. tail withdrawal procedure. In addition, maximum antinociceptive and discriminative stimulus effects of fixed-proportion fentanyl/naltrexone mixtures (1:0.018, 1:0.054, 1:0.18, 1:0.3, and 1:0.54) were used to quantify 1) the relative in vivo efficacy of the two GPB-MOR agonists and five unbiased MOR ligands, and 2) potential species differences in MOR ligand effects between rats and monkeys. The efficacy-effect function generated from the fentanyl/naltrexone mixtures stratified the five unbiased ligands consistent with agonist-stimulated GTPγS binding (NAQ = nalbuphine buprenorphine morphine methadone). However, TRV130 and SR-14968 produced greater antinociception and less fentanyl-like stimulus effects than was predicted. Furthermore, there was a significant positive correlation between rat and monkey antinociceptive effects. Overall, these results demonstrate GPB-MOR agonists produce undesirable abuse-related effects, albeit with slightly better potency and efficacy ratios compared to unbiased agonists. This article is part of the Special Issue entitled 'Opioid Neuropharmacology: Advances in treating pain and opioid addiction'.

Published

2019

28. Core Outcome Measures in Preclinical Assessment of Candidate Analgesics

Author

S. Stevens Negus

Subjects

0301 basic medicine, medicine.medical_specialty, Analgesic, Drug Evaluation, Preclinical, MEDLINE, Pain, Disease, 03 medical and health sciences, 0302 clinical medicine, Physical medicine and rehabilitation, Drug Discovery, Outcome Assessment, Health Care, medicine, Animals, Humans, Pharmacological modulation, Review Articles, Pharmacology, Analgesics, Behavior, Animal, business.industry, Outcome measures, Pain stimulus, Disease Models, Animal, 030104 developmental biology, Preclinical testing, Conditioning, Operant, Molecular Medicine, Pain behavior, business, 030217 neurology & neurosurgery

Abstract

All preclinical procedures for analgesic drug discovery involve two components: 1) a “pain stimulus” (the principal independent variable), which is delivered to an experimental subject with the intention of producing a pain state; and 2) a “pain behavior” (the principal dependent variable), which is measured as evidence of that pain state. Candidate analgesics are then evaluated for their effectiveness to reduce the pain behavior, and results are used to prioritize drugs for advancement to clinical testing. This review describes a taxonomy of preclinical procedures organized into an “antinociception matrix” by reference to their types of pain stimulus (noxious, inflammatory, neuropathic, disease related) and pain behavior (unconditioned, classically conditioned, operant conditioned). Particular emphasis is devoted to pain behaviors and the behavioral principals that govern their expression, pharmacological modulation, and preclinical-to-clinical translation. Strengths and weaknesses are compared and contrasted for procedures using each type of behavioral outcome measure, and the following four recommendations are offered to promote strategic use of these procedures for preclinical-to-clinical analgesic drug testing. First, attend to the degree of homology between preclinical and clinical outcome measures, and use preclinical procedures with behavioral outcome measures homologous to clinically relevant outcomes in humans. Second, use combinations of preclinical procedures with complementary strengths and weaknesses to optimize both sensitivity and selectivity of preclinical testing. Third, take advantage of failed clinical translation to identify drugs that can be back-translated preclinically as active negative controls. Finally, increase precision of procedure labels by indicating both the pain stimulus and the pain behavior in naming preclinical procedures.

Published

2019

29. Sex differences in opioid reinforcement under a fentanyl vs. food choice procedure in rats

Author

S. Stevens Negus, S. Barak Caine, E. Andrew Townsend, Morgane Thomsen, and Matthew L. Banks

Subjects

Pharmacology, Clinical literature, 030227 psychiatry, Fentanyl, 03 medical and health sciences, Psychiatry and Mental health, 0302 clinical medicine, Opioid, Clinical evidence, Anesthesia, Food choice, medicine, Economic analysis, Reinforcement, 030217 neurology & neurosurgery, Sex characteristics, medicine.drug

Abstract

Clinical evidence suggest that men are more sensitive than women to the abuse-related effects of mu-opioid agonists. In contrast, preclinical studies suggest the opposite sex difference. The aim of the present study was to clarify this discrepancy using a fentanyl vs. diluted Ensure® choice procedure to assess sex differences in opioid reinforcement. Sex differences in intravenous (IV) fentanyl self-administration were examined under a fixed-ratio (FR5) schedule, a multi-day progressive-ratio (PR) schedule for behavioral economic analysis, and a concurrent (choice) schedule of fentanyl and diluted Ensure® reinforcement in Sprague–Dawley male and female rats. The fentanyl dose-effect function under the FR5 schedule was significantly shifted upward in females compared to males. Similarly, the reinforcing effectiveness of both fentanyl (3.2 and 10 µg/kg per injection, IV) and diluted Ensure® (18 and 56%) were greater in females than in males as assessed using behavioral economic analysis, irrespective of dose or concentration. However, under a fentanyl vs. foodchoice procedure, males chose 3.2 µg/kg per injection fentanyl injections over 18%, but not 56%, diluted Ensure® at a higher percentage compared to females. Overall, these results suggest that the expression of sex differences in opioid reinforcement depends upon the schedule of reinforcement and that preclinical opioid vs. food choice procedures provide a translationally relevant measure (i.e., behavioral allocation) consistent with the direction of sex differences reported in the clinical literature.

Published

2019

30. Determinants of opioid abuse potential: Insights using intracranial self-stimulation

Author

Megan J. Moerke and S. Stevens Negus

Subjects

Agonist, Physiology, medicine.drug_class, 030209 endocrinology & metabolism, Stimulation, Pharmacology, Biochemistry, Article, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, Self Stimulation, 0302 clinical medicine, Endocrinology, medicine, Animals, business.industry, Opioid abuse, Opioid-Related Disorders, Electric Stimulation, Rats, Analgesics, Opioid, Opioid, Facilitation, Morphine, μ-opioid receptor, business, 030217 neurology & neurosurgery, Electrical brain stimulation, medicine.drug

Abstract

Intracranial self-stimulation (ICSS) is one procedure that can be used for preclinical abuse potential assessment. In ICSS procedures, subjects with microelectrodes implanted into a brain-reward region are trained to press an operant response lever for pulses of electrical brain stimulation, and drugs are evaluated for their effectiveness to increase or “facilitate” ICSS responding (an abuse-related effect) or to depress ICSS responding (an abuse-limiting effect). ICSS has been used for decades to evaluate determinants of opioid abuse potential, and this article reviews pharmacological and biological determinants of opioid abuse potential as revealed by ICSS studies in rodents. One of the most important observations from ICSS studies is that abused mu opioid receptor (MOR) agonists like morphine often fail to produce abuse-related ICSS facilitation in opioid-naïve subjects, but several days of repeated opioid exposure is sufficient for opioid-induced facilitation to emerge. Future studies with ICSS could help (a) to clarify mechanisms that increase MOR agonist abuse potential during early opioid exposure or during chronic exposure leading to dependence, (b) to evaluate novel opioids either developed as candidate analgesics with reduced abuse potential or identified as designer opioids being synthesized and distributed for illicit use, and (c) to test candidate pharmacotherapies for treatment of opioid abuse in non-dependent and dependent subjects.

Published

2019

31. Lack of effect of different pain-related manipulations on opioid self-administration, reinstatement of opioid seeking, and opioid choice in rats

Author

S. Stevens Negus, Javier Orihuel, E. Andrew Townsend, Sarah M Claypool, David J. Reiner, Yavin Shaham, Sarah V. Applebey, and Matthew L. Banks

Subjects

Male, Drug-Seeking Behavior, Pain, Self Administration, Pharmacology, Choice Behavior, Article, Heroin, Fentanyl, Extinction, Psychological, 03 medical and health sciences, 0302 clinical medicine, Noxious stimulus, medicine, Animals, Pain Measurement, business.industry, Chronic pain, Extinction (psychology), medicine.disease, Opioid-Related Disorders, 030227 psychiatry, Rats, Analgesics, Opioid, Nociception, Opioid, Conditioning, Operant, Female, Self-administration, business, Reinforcement, Psychology, 030217 neurology & neurosurgery, medicine.drug

Abstract

Rationale and ObjectivePain-related factors increase risk for opioid addiction, and opioid-induced pain relief may function as a negative reinforcer to increase opioid taking and seeking. However, experimental pain-related manipulations generally do not increase opioid self-administration in rodents. This discrepancy may reflect insufficient learning of pain-relief contingencies or confounding effects of pain-related behavioral impairments. Here we determined if pairing noxious stimuli with opioid self-administration would promote pain-related reinstatement of opioid seeking or increase opioid choice over food.MethodsIn Experiment 1, rats self-administered fentanyl in the presence or absence of repeated intraplantar capsaicin injections in distinct contexts to model context-specific exposure to cutaneous nociception. After capsaicin-free extinction in both contexts, we tested if capsaicin would reinstate fentanyl seeking. In Experiment 2, rats self-administered heroin after intraperitoneal (i.p.) lactic acid injections to model acute visceral inflammatory pain. After lactic acid-free extinction, we tested if lactic acid would reinstate heroin seeking. In Experiment 3, we tested if repeated i.p. lactic acid or intraplantar Complete Freund’s Adjuvant (CFA; to model sustained inflammatory pain) would increase fentanyl choice over food.ResultsIn Experiments 1-2, neither capsaicin nor lactic acid reinstated opioid seeking after extinction, and lactic acid did not increase heroin-induced reinstatement. In Experiment 3, lactic acid and CFA decreased reinforcement rate without affecting fentanyl choice.ConclusionsResults extend the range of conditions across which pain-related manipulations fail to increase opioid seeking in rats and suggest that enhanced opioid-addiction risk in humans with chronic pain involves factors other than enhanced opioid reinforcement and relapse.

Published

2021

32. Temporal parameters of enhanced opioid reward after initial opioid exposure in rats

Author

S. Stevens Negus and Megan J. Moerke

Subjects

Male, Time Factors, Receptors, Opioid, mu, Pain, Article, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Self Stimulation, Reward, medicine, Effective treatment, Animals, Dosing, Pharmacology, Morphine, business.industry, Morphine treatment, Brain, Mu-Opioid Receptor Agonists, Electric Stimulation, 030227 psychiatry, Rats, Analgesics, Opioid, Regimen, Opioid, Anesthesia, business, 030217 neurology & neurosurgery, Electrical brain stimulation, medicine.drug

Abstract

RATIONALE: Mu opioid receptor agonists are indispensable for the treatment of pain, but clinical use carries the inherent risk of transition from effective treatment to abuse. Abuse potential appears to increase rapidly during periods of initial opioid exposure in humans, and this increase in opioid reward during initial opioid exposure can be modeled in rats using an intracranial self-stimulation (ICSS) procedure. OBJECTIVES: The goal of the present study was to examine temporal parameters of this phenomenon. METHODS: Adult male Sprague-Dawley rats responded for electrical brain stimulation using a frequency-rate ICSS procedure. In the first experiment, rats received daily morphine injections for six days, and morphine effects on ICSS were redetermined one day, one week, or one month after the repeated-morphine treatment regimen to evaluate the persistence of enhanced opioid reward. In the second experiment, rats received six repeated morphine injections with different interdose intervals (two per day, one per day, every other day, every fourth day), and morphine effects were redetermined one day after the last dose to determine dosing frequencies sufficient to produce enhanced opioid reward. RESULTS: Results of the first experiment indicated that enhanced opioid reward was greatest one day after the morphine-treatment regimen and completely dissipated after four weeks. The second experiment indicated that all dosing frequencies tested were sufficient to produce enhanced reward. CONCLUSIONS: Taken together, these results suggest that enhancement of opioid reward after initial opioid exposure is relatively transient but can be produced by a range of different dosing frequencies.

Published

2021

33. Expression and Treatment of Pain-Depressed Climbing in Male and Female Mice

Author

Edna J. Santos, Arianna Giddings, Farah Kandil, and S. Stevens Negus

Subjects

Anesthesiology and Pain Medicine, Neurology, Neurology (clinical)

Published

2022

34. Manipulating Pharmacodynamic Efficacy with Agonist + Antagonist Mixtures: In Vitro and In Vivo Studies with Opioids and Cannabinoids

Author

Dana E. Selley, Clare M Diester, S. Stevens Negus, Abdul M Jali, Luke P Legakis, Matthew L. Banks, and Edna J Santos

Subjects

0301 basic medicine, Agonist, Male, medicine.drug_class, medicine.medical_treatment, Receptors, Opioid, mu, CHO Cells, Pharmacology, 03 medical and health sciences, Mice, 0302 clinical medicine, Cricetulus, Rimonabant, Receptor, Cannabinoid, CB1, In vivo, medicine, Inverse agonist, Animals, Drug Interactions, Receptor, Dose-Response Relationship, Drug, Chemistry, Cannabinoids, Antagonist, Analgesics, Opioid, 030104 developmental biology, Behavioral Pharmacology, Molecular Medicine, Cannabinoid, Receptor theory, 030217 neurology & neurosurgery, medicine.drug

Abstract

Pharmacodynamic efficacy of drugs to activate their receptors is a key determinant of drug effects, and intermediate-efficacy agonists are often useful clinically because they retain sufficient efficacy to produce therapeutically desirable effects while minimizing undesirable effects. Molecular mechanisms of efficacy are not well understood, so rational drug design to control efficacy is not yet possible; however, receptor theory predicts that fixed-proportion mixtures of an agonist and antagonist for a given receptor can be adjusted to precisely control net efficacy of the mixture in activating that receptor. Moreover, the agonist proportion required to produce different effects provides a quantitative scale for comparing efficacy requirements across those effects. To test this hypothesis, the present study evaluated effectiveness of fixed-proportion agonist/antagonist mixtures to produce in vitro and in vivo effects mediated by μ-opioid receptors (MOR) and cannabinoid type 1 receptors (CB(1)R). Mixtures of 1) the MOR agonist fentanyl and antagonist naltrexone and 2) the CB(1)R agonist CP55,940 and antagonist/inverse agonist rimonabant were evaluated in an in vitro assay of ligand-stimulated guanosine 5′-O-(3-[(35)S]thio)triphosphate binding and an in vivo assay of thermal nociception in mice. For both agonist/antagonist pairs in both assays, increasing agonist proportions produced graded increases in maximal mixture effects, and lower agonist proportions were sufficient to produce in vivo than in vitro effects. These findings support the utility of agonist-antagonist mixtures as a strategy to control net efficacy of receptor activation and to quantify and compare efficacy requirements across a range of in vitro and in vivo endpoints. SIGNIFICANCE STATEMENT: Manipulation of agonist proportion in agonist/antagonist mixtures governs net mixture efficacy at the target receptor. Parameters of agonist/antagonist mixture effects can provide a quantitative metric for comparison of efficacy requirements across a wide range of conditions.

Published

2020

35. Factors mediating pain-related risk for opioid use disorder

Author

S. Stevens Negus, Arbi Nazarian, and Thomas J. Martin

Subjects

0301 basic medicine, medicine.medical_specialty, Vulnerability, Context (language use), Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Risk Factors, Conditioning, Psychological, medicine, Animals, Humans, Psychiatry, Pharmacology, business.industry, Chronic pain, Cognition, Opioid use disorder, medicine.disease, Opioid-Related Disorders, Social relation, Substance abuse, Analgesics, Opioid, 030104 developmental biology, Opioid, Chronic Pain, business, Reinforcement, Psychology, 030217 neurology & neurosurgery, medicine.drug

Abstract

Pain is a complex experience with far-reaching organismal influences ranging from biological factors to those that are psychological and social. Such influences can serve as pain-related risk factors that represent susceptibilities to opioid use disorder. This review evaluates various pain-related risk factors to form a consensus on those that facilitate opioid abuse. Epidemiological findings represent a high degree of co-occurrence between chronic pain and opioid use disorder that is, in part, driven by an increase in the availability of opioid analgesics and the diversion of their use in a non-medical context. Brain imaging studies in individuals with chronic pain that use/abuse opioids suggest abuse-related mechanisms that are rooted within mesocorticolimbic processing. Preclinical studies suggest that pain states have a limited impact on increasing the rewarding effects of opioids. Indeed, many findings indicate a reduction in the rewarding and reinforcing effects of opioids during pain states. An increase in opioid use may be facilitated by an increase in the availability of opioids and a decrease in access to non-opioid reinforcers that require mobility or social interaction. Moreover, chronic pain and substance abuse conditions are known to impair cognitive function, resulting in deficits in attention and decision making that may promote opioid abuse. A better understanding of pain-related risk factors can improve our knowledge in the development of OUD in persons with pain conditions and can help identify appropriate treatment strategies. This article is part of the special issue on ‘Vulnerabilities to Substance Abuse.’.

Published

2020

36. Learning from lorcaserin: lessons from the negative clinical trial of lorcaserin to treat cocaine use disorder

Author

S. Stevens Negus and Matthew L. Banks

Subjects

Pharmacology, medicine.medical_specialty, Clinical Trials as Topic, Extramural, business.industry, MEDLINE, Benzazepines, Lorcaserin, Clinical trial, Psychiatry and Mental health, Cocaine, Perspective, medicine, Cocaine use, Humans, Psychiatry, business, Serotonin 5-HT2 Receptor Agonists, medicine.drug

Published

2020

37. An investigation of the optical isomers of methcathinone (MCAT), and two achiral analogs, at monoamine transporters and in intracranial self- stimulation studies in rats

Author

Farhana Sakloth, Rachel A. Davies, Vy T. Nguyen, Tyson R. Baird, Brian Ruiz, Richard A. Glennon, Jose M. Eltit, and S. Stevens Negus

Subjects

Physiology, Stereochemistry, Cognitive Neuroscience, Synthetic cathinone, Stimulation, Biochemistry, Methcathinone, Article, 03 medical and health sciences, 0302 clinical medicine, Self Stimulation, Central Stimulants, medicine, Animals, 030304 developmental biology, Serotonin Plasma Membrane Transport Proteins, 0303 health sciences, Dopamine Plasma Membrane Transport Proteins, Propiophenones, Norepinephrine Plasma Membrane Transport Proteins, Chemistry, Transporter, Cell Biology, General Medicine, Rats, Monoamine neurotransmitter, 030217 neurology & neurosurgery, medicine.drug

Abstract

Methcathinone (MCAT; 1), the progenitor of numerous and widely abused “synthetic cathinone” central stimulants, exists as a pair of optical isomers. Although S(−)MCAT is several-fold more potent than R(+)MCAT in rodent locomotor stimulation and in stimulus generalization studies in rat drug discrimination assays, the individual optical isomers of MCAT have never been directly compared for their actions at monoamine transporters that seem to underlie their actions, and have never been examined for their relative abuse potential. Here, we found that the isomers of MCAT are nearly equi-effective at dopamine and norepinephrine transporters (DAT and NET, respectively) as transporter substrates (i.e., as releasing agents), and are ≥63-fold less potent at the serotonin transporter (SERT). In intracranial self-stimulation (ICSS) studies to evaluate abuse-related drug effects in rats, S(−)MCAT was approximately twice as potent as its R-enantiomer. Achiral analogs, α-methyl MCAT (3) and α-des-methyl MCAT (4), also were DAT/NET substrates and also produced abuse-related ICSS effects, indicating that they retain abuse potential and that they might be useful for the further study of the stereochemistry of synthetic cathinone analogs with chiral β- (or other) substituents.

Published

2020

38. Addressing the Opioid Crisis: The Importance of Choosing Translational Endpoints in Analgesic Drug Discovery

Author

S. Stevens Negus

Subjects

0301 basic medicine, medicine.medical_specialty, Functional impairment, Analgesic, Pain, Translational research, Toxicology, Article, Translational Research, Biomedical, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, medicine, Animals, Humans, Intensive care medicine, Depression (differential diagnoses), Pharmacology, Analgesics, Drug discovery, business.industry, Opioid-Related Disorders, Analgesics, Opioid, 030104 developmental biology, Drug development, Opioid, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

The opioid crisis has stimulated renewed interest in analgesic drug development. This effort will involve preclinical-to-clinical translational research and will benefit from a focus on endpoints that are both clinically relevant and shared across laboratory animals and humans. Measures of pain-related functional impairment and behavioral depression could serve this purpose.

Published

2018

39. Modulation of drug choice by extended drug access and withdrawal in rhesus monkeys: Implications for negative reinforcement as a driver of addiction and target for medications development

Author

S. Stevens Negus and Matthew L. Banks

Subjects

0301 basic medicine, Narcotic Antagonists, media_common.quotation_subject, Clinical Biochemistry, Pharmacology, Toxicology, Choice Behavior, Biochemistry, κ-opioid receptor, Dopamine agonist, Article, Heroin, Cocaine-Related Disorders, 03 medical and health sciences, Behavioral Neuroscience, 0302 clinical medicine, Cocaine, medicine, Animals, Humans, Biological Psychiatry, media_common, Heroin Dependence, Addiction, Opioid use disorder, Opioid-Related Disorders, medicine.disease, Macaca mulatta, Substance Withdrawal Syndrome, Disease Models, Animal, 030104 developmental biology, Food, μ-opioid receptor, Psychology, Reinforcement, Psychology, 030217 neurology & neurosurgery, medicine.drug, Methadone, Buprenorphine

Abstract

Chronic drug exposure is hypothesized to recruit negative reinforcement processes that increase the magnitude and alter the mechanisms of drug reinforcement. Candidate substrates of negative reinforcement include increased signaling via stress-related neurotransmitters such as corticotropin releasing factor (CRF, acting at CRF receptors) or dynorphin (acting at kappa opioid receptors) and/or decreased signaling via reward-related neurotransmitters such as dopamine. Determinants of drug reinforcement can be examined with choice procedures, in which subjects choose between a drug of interest (e.g. heroin or cocaine) and a non-drug alternative reinforcer (e.g. food). This review summarizes evidence collected from studies of drug choice in rhesus monkeys to address the negative reinforcement hypothesis. In monkeys choosing between heroin and food, chronic heroin exposure and subsequent withdrawal produces a robust increase in heroin choice. This withdrawal-associated increase in heroin choice is blocked by morphine and by other mu opioid agonists used to treat opioid use disorder (methadone, buprenorphine); however, withdrawal-associated increases in heroin choice are not reliably blocked by antagonists of CRF or kappa opioid receptors or by an indirect dopamine agonist. In monkeys choosing between cocaine and food, chronic cocaine exposure and withdrawal fail to increase cocaine choice or alter sensitivity of cocaine choice to treatment with candidate therapeutics including an indirect dopamine agonist and a kappa opioid receptor antagonist. These results support a role for negative reinforcement in self-administration of heroin but not cocaine. The constellation of neurobiological changes that constitutes the negative reinforcing stimulus in opioid-dependent rhesus monkeys remains to be determined.

Published

2018

40. Maintenance on naltrexone + amphetamine decreases cocaine-vs.-food choice in male rhesus monkeys

Author

Megan J. Moerke, S. Stevens Negus, Kenner C. Rice, Kejun Cheng, and Matthew L. Banks

Subjects

Male, Agonist, Dextroamphetamine, medicine.drug_class, Receptors, Opioid, mu, Self Administration, Pharmacology, Toxicology, Choice Behavior, Article, Naltrexone, 03 medical and health sciences, 0302 clinical medicine, Cocaine, Opioid receptor, medicine, Animals, Drug Interactions, Pharmacology (medical), Amphetamine, Endogenous opioid, Dose-Response Relationship, Drug, Morphine, business.industry, Antagonist, Macaca mulatta, 030227 psychiatry, Psychiatry and Mental health, Food, Anesthesia, Administration, Intravenous, business, Reinforcement, Psychology, 030217 neurology & neurosurgery, Opioid antagonist, medicine.drug

Abstract

Background Cocaine use disorder remains a significant public health issue for which there are no FDA-approved pharmacotherapies. Amphetamine maintenance reduces cocaine use in preclinical and clinical studies, but the mechanism of this effect is unknown. Previous studies indicate a role for endogenous opioid release and subsequent opioid receptor activation in some amphetamine effects; therefore, the current study examined the role of mu-opioid receptor activation in d-amphetamine treatment effects in an assay of cocaine-vs-food choice. Methods Adult male rhesus monkeys with double-lumen intravenous catheters responded for concurrently available food pellets and cocaine injections (0–0.1 mg/kg/injection) during daily sessions. Cocaine choice and overall reinforcement rates were evaluated during 7-day treatments with saline or test drugs. Results During saline treatment, cocaine maintained a dose-dependent increase in cocaine-vs.-food choice. The mu-opioid receptor agonist morphine (0.032–0.32 mg/kg/h) dose-dependently increased cocaine choice and decreased rates of reinforcement. A dose of the mu-selective opioid receptor antagonist naltrexone (0.0032 mg/kg/h) that completely blocked morphine effects had no effect on cocaine choice when it was administered alone, but it enhanced the effectiveness of a threshold dose of 0.032 mg/kg/h amphetamine to decrease cocaine choice without also enhancing nonselective behavioral disruption by this dose of amphetamine. Conversely, the kappa-selective opioid antagonist norbinalorphimine did not enhance amphetamine effects on cocaine choice. Conclusions These results suggest that amphetamine maintenance produces mu opioid-receptor mediated effects that oppose its anti-cocaine effects. Co-administration of naltrexone may selectively enhance amphetamine potency to decrease cocaine choice without increasing amphetamine potency to produce general behavioral disruption.

Published

2017

41. Dissociable effects of the kappa opioid receptor agonist nalfurafine on pain/itch-stimulated and pain/itch-depressed behaviors in male rats

Author

F. Ivy Carroll, Megan J. Moerke, S. Stevens Negus, E. Andrew Townsend, Kevin B. Freeman, and Matthew L. Lazenka

Subjects

Male, 0301 basic medicine, Agonist, medicine.medical_specialty, Uremic pruritus, medicine.drug_class, Pain, Pharmacology, κ-opioid receptor, Article, Rats, Sprague-Dawley, 03 medical and health sciences, Self Stimulation, 0302 clinical medicine, Japan, Internal medicine, medicine, Animals, Spiro Compounds, 5-HT receptor, Behavior, Animal, Dose-Response Relationship, Drug, Depression, business.industry, Pruritus, Receptors, Opioid, kappa, Scratching, medicine.disease, Rats, Analgesics, Opioid, 030104 developmental biology, Nociception, Endocrinology, Morphinans, Serotonin, business, 030217 neurology & neurosurgery, Nalfurafine, medicine.drug

Abstract

Nalfurafine is a G protein signaling-biased kappa opioid receptor (KOR) agonist approved in Japan for second-line treatment of uremic pruritus. Neither nalfurafine nor any other KOR agonist is currently approved anywhere for treatment of pain, but recent evidence suggests that G protein signaling-biased KOR agonists may have promise as candidate analgesics/antipruritics with reduced side effects compared to nonbiased or s-arrestin-signaling-biased KOR agonists. This study compared nalfurafine effects in rats using assays of pain-stimulated and pain-depressed behavior used previously to evaluate other candidate analgesics. Nalfurafine effects were also examined in complementary assays of itch-stimulated and itch-depressed behavior. Intraperitoneal lactic acid (IP acid) and intradermal serotonin (ID 5HT) served as noxious and pruritic stimuli, respectively, in male Sprague Dawley rats to stimulate stretching (IP acid) or scratching (ID 5HT) or to depress positively reinforced operant responding in an assay of intracranial self-stimulation (ICSS; both stimuli). Nalfurafine was equipotent to decrease IP acid-stimulated stretching and ID 5HT-stimulated scratching; however, doses of nalfurafine that decreased these pain/itch-stimulated behaviors also decreased control ICSS performance. Moreover, nalfurafine failed to alleviate either IP acid- or ID 5HT-induced depression of ICSS. These results suggest that nalfurafine-induced decreases in pain/itch-stimulated behaviors may reflect nonselective decreases in motivated behavior rather than analgesia or antipruritus against the noxious and pruritic stimuli used here. This conclusion agrees with the absence of clinical data for nalfurafine analgesia and the weak clinical data for nalfurafine antipruritus. Nalfurafine bias for G protein signaling may not be sufficient for clinically safe and reliable analgesia or antipruritus.

Published

2017

42. Effects of nalfurafine on the reinforcing, thermal antinociceptive, and respiratory-depressant effects of oxycodone: modeling an abuse-deterrent opioid analgesic in rats

Author

Hina N. Qureshi, Kenneth J. Sufka, Jussara M. do Carmo, Coco N. Kapanda, Hunter W. McLendon, Fernanda S. da Silva, John E. Hall, S. Stevens Negus, Jennifer E. Naylor, E. Andrew Townsend, Kevin B. Freeman, Shelley R. Edwards, and Christopher R. McCurdy

Subjects

Male, Nociception, 0301 basic medicine, Agonist, medicine.drug_class, Receptors, Opioid, mu, Self Administration, Pharmacology, Article, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Spiro Compounds, Analgesics, Dose-Response Relationship, Drug, business.industry, Respiration, Opioid-Related Disorders, Rats, Analgesics, Opioid, 030104 developmental biology, Morphinans, Opioid, Models, Animal, Depressant, μ-opioid receptor, Self-administration, business, Reinforcement, Psychology, Oxycodone, 030217 neurology & neurosurgery, Nalfurafine, medicine.drug

Abstract

Strategies to reduce the misuse of mu opioid agonists are critically needed. Previous work has shown that kappa opioid agonists can diminish the abuse-related effects and augment the antinociceptive effects of mu agonists. However, use of traditional kappa agonists is limited by their dysphoric side effects. The current study examined the effects of nalfurafine, a clinically available atypical kappa agonist, on the reinforcing, thermal antinociceptive, and respiratory-depressant effects of oxycodone in male rats. To determine oxycodone/nalfurafine mixture proportions to be examined intravenously across procedures, a progressive ratio (PR) self-administration procedure compared the reinforcing effects of oxycodone (56 μg/kg/inj) available alone or as a mixture with co-administered nalfurafine (0.32, 1, or 3.2 μg/kg/inj), corresponding to oxycodone/nalfurafine proportions of 175:1, 56:1, and 18:1, respectively. Next, PR and thermal antinociception dose-effect functions were each determined for oxycodone, nalfurafine, and the same oxycodone/nalfurafine mixture proportions. Finally, the respiratory-depressant effects of equi-antinociceptive doses of oxycodone, nalfurafine, and the mixtures were compared. Nalfurafine decreased the reinforcing effects of oxycodone, and the 18:1 mixture did not function as a reinforcer. Oxycodone and nalfurafine each produced dose-dependent antinociception, and the mixtures produced additive antinociception. In addition, antinociceptive doses of the 56:1 and 18:1 mixtures did not produce respiratory depression. These results suggest that nalfurafine may augment the thermal antinociceptive effects while reducing the reinforcing and respiratory-depressant effects of oxycodone.

Published

2017

43. N-Alkylated Analogs of 4-Methylamphetamine (4-MA) Differentially Affect Monoamine Transporters and Abuse Liability

Author

Michael H. Baumann, John S. Partilla, S. Stevens Negus, Farhana Sakloth, Ernesto Solis, Kathryn L. Schwienteck, Iwona Ruchala, Louis J. De Felice, Richard A. Glennon, and Jose M. Eltit

Subjects

Male, 0301 basic medicine, Serotonin, Alkylation, Dopamine, Amphetamine-Related Disorders, Pharmacology, Membrane Potentials, Rats, Sprague-Dawley, 4-Methylamphetamine, Norepinephrine, Xenopus laevis, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Membrane Transport Modulators, Calcium flux, medicine, Animals, Humans, Voltage-dependent calcium channel, Chemistry, Amphetamines, Brain, Transporter, Psychiatry and Mental health, HEK293 Cells, 030104 developmental biology, Monoamine neurotransmitter, Biochemistry, Vesicular Monoamine Transport Proteins, Oocytes, Original Article, Calcium, Calcium Channels, 030217 neurology & neurosurgery, Synaptosomes, medicine.drug

Abstract

Clandestine chemists synthesize novel stimulant drugs by exploiting structural templates known to target monoamine transporters for dopamine, norepinephrine, and serotonin (DAT, NET, and SERT, respectively). 4-Methylamphetamine (4-MA) is an emerging drug of abuse that interacts with transporters, but limited structure-activity data are available for its analogs. Here we employed uptake and release assays in rat brain synaptosomes, voltage-clamp current measurements in cells expressing transporters, and calcium flux assays in cells coexpressing transporters and calcium channels to study the effects of increasing N-alkyl chain length of 4-MA on interactions at DAT, NET, and SERT. In addition, we performed intracranial self-stimulation in rats to understand how the chemical modifications affect abuse liability. All 4-MA analogs inhibited uptake at DAT, NET, and SERT, but lengthening the amine substituent from methyl to ethyl, propyl, and butyl produced a stepwise decrease in potency. N-methyl 4-MA was an efficacious substrate-type releaser at DAT that evoked an inward depolarizing current and calcium influx, whereas other analogs did not exhibit these effects. N-methyl and N-ethyl 4-MA were substrates at NET, whereas N-propyl and N-butyl 4-MA were not. All analogs acted as SERT substrates, though N-butyl 4-MA had very weak effects. Intracranial self-stimulation in rats showed that elongating the N-alkyl chain decreased abuse-related effects in vivo that appeared to parallel reductions in DAT activity. Overall, converging lines of evidence show that lengthening the N-alkyl substituent of 4-MA reduces potency to inhibit transporters, eliminates substrate activity at DAT and NET, and decreases abuse liability of the compounds.

Published

2017

44. Effects of Acute and Chronic Treatments with Dopamine D2 and D3 Receptor Ligands on Cocaine versus Food Choice in Rats

Author

S. Stevens Negus, Paul Butler, Andrew C. Barrett, S. Barak Caine, and Morgane Thomsen

Subjects

Pharmacology, Drug, Agonist, medicine.drug_class, media_common.quotation_subject, Addiction, Antagonist, Terguride, Partial agonist, 030227 psychiatry, 03 medical and health sciences, 0302 clinical medicine, Dopamine receptor D3, Dopamine receptor D2, medicine, Molecular Medicine, Psychology, 030217 neurology & neurosurgery, media_common, medicine.drug

Abstract

Dopamine D3 receptor ligands are potential medications for psychostimulant addiction. Medication assessment may benefit from preclinical studies that evaluate chronic medication effects on choice between an abused drug and an alternative, nondrug reinforcer. This study compared acute and chronic effects of dopamine D2- and D3-preferring ligands on choice between intravenous cocaine and palatable food in rats. Under baseline conditions, cocaine maintained dose-dependent increases in cocaine choice and reciprocal decreases in food choice. Acutely, the D2 agonist R-(−)-norpropylapomorphine (NPA) and antagonist L-741,626 [3-[[4-(4-chlorophenyl)-4-hydroxypiperidin-l-yl]methyl-1H-indole] produced leftward and rightward shifts in cocaine dose-effect curves, respectively, whereas the partial agonist terguride had no effect. All three drugs dose-dependently decreased food-maintained responding. Chronically, the effects of R-(−)-norpropylapomorphine and L-741,626 on cocaine self-administration showed marked tolerance, whereas suppression of food-reinforced behavior persisted. Acute effects of the D3 ligands were less systematic and most consistent with nonselective decreases in cocaine- and food-maintained responding. Chronically, the D3 agonist PF-592,379 [5-[(2R,5S)-5-methyl-4-propylmorpholin-2-yl]pyridin-2-amine] increased cocaine choice, whereas an intermediate dose of the D3 antagonist PG01037 [N-[(E)-4-[4-(2,3-dichlorophenyl)piperazin-1-yl]but-2-enyl]-4-pyridin-2-ylbenzamide] produced a therapeutically desirable decrease in cocaine choice early in treatment; however, tolerance to this effect developed, and lower and higher doses were ineffective. D3 ligands failed to significantly modify total cocaine intake but caused persistent decreases in food intake. Thus, D2-and D3-preferring ligands showed distinct profiles, consistent with different pharmacological actions. In addition, these results highlight the role of acute versus chronic treatment as a determinant of test drug effects. With the possible exception of the D3 antagonist PG01037, no ligand was promising in terms of cocaine addiction treatment.

Published

2017

45. Role of d -amphetamine and d -methamphetamine as active metabolites of benzphetamine: Evidence from drug discrimination and pharmacokinetic studies in male rhesus monkeys

Author

S. Stevens Negus, Rodney W. Snyder, Timothy R. Fennell, and Matthew L. Banks

Subjects

Male, Agonist, Dextroamphetamine, medicine.drug_class, Clinical Biochemistry, Pharmacology, Toxicology, Biochemistry, Article, Methamphetamine, 03 medical and health sciences, Behavioral Neuroscience, 0302 clinical medicine, Pharmacokinetics, medicine, Animals, Potency, Amphetamine, Biological Psychiatry, Active metabolite, Behavior, Animal, Benzphetamine, Macaca mulatta, 030227 psychiatry, Pharmacodynamics, Anorectic, Psychology, 030217 neurology & neurosurgery, medicine.drug

Abstract

Benzphetamine is a Schedule III anorectic agent that is a prodrug for d-amphetamine and d-methamphetamine and may have utility as an “agonist” medication for cocaine use disorder treatment. This study evaluated the pharmacokinetic-pharmacodynamic profile of benzphetamine using a drug discrimination procedure in rhesus monkeys. The potency and time course of cocaine-like discriminative stimulus effects were compared for benzphetamine (10–18 mg/kg, intramuscular (IM)) and d-amphetamine (0.032–0.32 mg/kg, IM) in monkeys (n=3–4) trained to discriminate IM cocaine (0.32 mg/kg) from saline in a two-key food-reinforced discrimination procedure. Parallel pharmacokinetic studies in the same monkeys determined plasma benzphetamine, d-methamphetamine and/or d-amphetamine levels for correlation with behavioral effects. d-Amphetamine produced dose-dependent, time-dependent, and full cocaine-like effects, i.e. ≥ 90% cocaine-appropriate responding,in all monkeys without altering response rates. The time course of d-amphetamine’s cocaine-like discriminative stimulus effects correlated with plasma d-amphetamine levels. Benzphetamine was 180-fold less potent than d-amphetamine and produced full cocaine-like effects in only 2 of 4 monkeys while significantly decreasing response rates. Benzphetamine administration increased plasma d-methamphetamine (peak at 100 min) and d-amphetamine (peak at 24 h) levels, but the time course of behavioral effects did not correlate with increased levels of benzphetamine, d-methamphetamine or d-amphetamine. These results suggest that benzphetamine yields d-amphetamine and d-methamphetamine as active metabolites in rhesus monkeys, but generation of these metabolites is not sufficient to account for benzphetamine behavioral effects. The incomplete cocaine substitution profile and protracted d-amphetamine plasma levels suggest that benzphetamine may still warrant further evaluation as a candidate pharmacotherapy for cocaine use disorder treatment.

Published

2017

46. Relief of Pain-Depressed Behavior in Rats by Activation of D1-Like Dopamine Receptors

Author

S. Stevens Negus, Matthew F. Lazenka, Kelen Freitas, and Sydney Henck

Subjects

Male, 0301 basic medicine, Agonist, medicine.medical_specialty, medicine.drug_class, Pain, Pharmacology, Rats, Sprague-Dawley, 03 medical and health sciences, Self Stimulation, 0302 clinical medicine, Quinpirole, Dopamine receptor D1, Dopamine Uptake Inhibitors, Dopamine, Internal medicine, medicine, Animals, Pain Management, Lactic Acid, Dopamine transporter, Analgesics, Behavior, Animal, Dose-Response Relationship, Drug, Pramipexole, biology, Depression, Receptors, Dopamine D1, Benzazepines, Sumanirole, Electrodes, Implanted, Rats, 030104 developmental biology, Endocrinology, Behavioral Pharmacology, Dopamine receptor, Dopamine Agonists, Methylphenidate, biology.protein, Conditioning, Operant, Molecular Medicine, Psychology, 030217 neurology & neurosurgery, medicine.drug

Abstract

Clinically significant pain often includes a decrease in both behavior and mesolimbic dopamine signaling. Indirect and/or direct dopamine receptor agonists may alleviate pain-related behavioral depression. To test this hypothesis, the present study compared effects of indirect and direct dopamine agonists in a preclinical assay of pain-depressed operant responding. Male Sprague-Dawley rats with chronic indwelling microelectrodes in the medial forebrain bundle were trained in an intracranial self-stimulation (ICSS) procedure to press a lever for pulses of electrical brain stimulation. Intraperitoneal injection of dilute lactic acid served as an acute noxious stimulus to depress ICSS. Intraperitoneal lactic acid-induced depression of ICSS was dose-dependently blocked by the dopamine transporter inhibitor methylphenidate and the D1-selective agonist SKF82958, but not by the D2/3-selective agonists quinpirole, pramipexole, or sumanirole. The antinociceptive effects of methylphenidate and SKF82958 were blocked by the D1-selective antagonist SCH39166. Acid-induced stimulation of a stretching response was evaluated in separate groups of rats, but all agonists decreased acid-stimulated stretching, and antagonism experiments were inconclusive due to direct effects of the antagonists when administered alone. Taken together, these results suggest that D1-receptor stimulation is both sufficient to block acid-induced depression of ICSS and necessary for methylphenidate antinociception in this procedure. Conversely, D2/3-receptor stimulation is not sufficient to relieve pain-depressed behavior. These results support the hypothesis that pain-related depression of dopamine D1 receptor signaling contributes to pain-related depression of behavior in rats. Additionally, these results support further consideration of indirect dopamine agonists and direct D1 receptor agonists as candidate treatments for pain-related behavioral depression.

Published

2017

47. Abuse-related effects of subtype-selective GABAA receptor positive allosteric modulators in an assay of intracranial self-stimulation in rats

Author

Guanguan Li, S. Stevens Negus, Kathryn L. Schwienteck, Michael M. Poe, Matthew L. Banks, and James M. Cook

Subjects

0301 basic medicine, Pharmacology, Zolpidem, business.industry, GABAA receptor, musculoskeletal, neural, and ocular physiology, Allosteric regulation, Stimulation, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, nervous system, Medicine, Medial forebrain bundle, business, Self-administration, Diazepam, 030217 neurology & neurosurgery, Electrical brain stimulation, medicine.drug

Abstract

GABAA positive allosteric modulators (GABAA PAMs), such as diazepam and zolpidem, are used clinically for anxiety and insomnia, but abuse liability is a concern. Novel GABAA PAMS may have lower abuse liability while retaining clinical utility. The present study compared abuse-related effects of the non-selective GABAA PAM diazepam, the α1-selective GABAA PAM zolpidem, and three novel GABAA PAMs (JY-XHe-053, XHe-II-053, and HZ-166) using intracranial self-stimulation (ICSS) in rats. These novel compounds have relatively low efficacy at α1-, α2-, and α3-containing GABAA receptors, putative in vivo selectivity at α2/α3-containing GABAA receptors, and produce anxiolytic-like effects with limited sedation in non-human primates. Adult, male Sprague-Dawley rats (n = 17) were each implanted with a bipolar electrode in the medial forebrain bundle and trained to respond under a fixed-ratio 1 schedule of reinforcement for electrical brain stimulation. The potency and time course of effects were compared for diazepam (0.1–10 mg/kg), zolpidem (0.032–3.2 mg/kg), and the three novel compounds (JY-XHe-053, XHe-II-053, and HZ-166; all 3.2–32 mg/kg). Zolpidem and diazepam produced transient facilitation of ICSS at small doses and more sustained rate-decreasing effects at larger doses. JY-XHe-053 and HZ-166 produced weak and inconsistent ICSS facilitation, whereas XHe-II-053 had no effect on ICSS. These results support a key role for α1-containing GABAA receptors in mediating GABAA PAM-induced ICSS facilitation. These results are concordant with drug self-administration studies in monkeys in suggesting that GABAA PAMs with low α1 efficacy and putative α2/α3 selectivity have lower abuse liability than high-efficacy non-selective or α1-selective GABAA PAMs.

Published

2017

48. Attenuated Dopamine Receptor Signaling in Nucleus Accumbens Core in a Rat Model of Chemically-Induced Neuropathy

Author

S. Stevens Negus, David N. Potter, William A. Carlezon, Matthew F. Lazenka, Dana E. Selley, Elena H. Chartoff, and Laura J. Sim-Selley

Subjects

medicine.medical_specialty, Tyrosine hydroxylase, Chemistry, Nucleus accumbens, Ventral tegmental area, Endocrinology, Allodynia, medicine.anatomical_structure, Dopamine, Dopamine receptor, Dopamine receptor D2, Internal medicine, medicine, medicine.symptom, Receptor, medicine.drug

Abstract

Neuropathy is major source of chronic pain that can be caused by mechanically or chemically induced nerve injury. Previous work in a rat model of neuropathic pain demonstrated that bilateral formalin injection into the hind paws produced mechanical hypersensitivity (allodynia) and depressed responding for intracranial self-stimulation (ICSS). To determine whether neuropathy alters dopamine receptor responsiveness in mesolimbic brain regions, we examined dopamine D1-like and D2-like receptor (D1/2R) signaling and expression in male rats 14 days after bilateral intraplantar formalin injections into both rear paws. D2R-mediated G-protein activation and expression of the D2R long, but not short, isoform were reduced in nucleus accumbens (NAc) core, but not in NAc shell, caudate-putamen (CPu) or ventral tegmental area (VTA) of formalin-compared to saline-treated rats. In addition, D1R-stimulated adenylyl cyclase (AC) activity was also reduced in NAc core, but not in NAc shell or prefrontal cortex, of formalin-treated rats, whereas D1R expression was unaffected. Expression of other proteins involved in dopamine neurotransmission, including dopamine uptake transporter (DAT) and tyrosine hydroxylase (TH), were unaffected by formalin treatment. In behavioral tests, the effects of D2R agonists on ICSS were attenuated in formalin-treated rats, whereas the effects of D1R agonists were unchanged. These results indicate that intraplantar formalin as a model of chemically induced neuropathy produces attenuation of highly specific DA receptor signaling processes in NAc core of male rats.

Published

2019

49. Lorcaserin maintenance fails to attenuate heroin vs. food choice in rhesus monkeys

Author

S. Stevens Negus, Matthew L. Banks, E. Andrew Townsend, and Justin L. Poklis

Subjects

Agonist, Male, medicine.drug_class, medicine.medical_treatment, Self Administration, Pharmacology, Toxicology, Choice Behavior, Naltrexone, Article, Lorcaserin, Heroin, 03 medical and health sciences, 0302 clinical medicine, Medicine, Animals, Pharmacology (medical), 030212 general & internal medicine, Saline, Dose-Response Relationship, Drug, business.industry, Opioid use disorder, Feeding Behavior, Benzazepines, medicine.disease, Macaca mulatta, 030227 psychiatry, 3. Good health, Analgesics, Opioid, Psychiatry and Mental health, Opioid, Female, business, 030217 neurology & neurosurgery, Opioid antagonist, medicine.drug

Abstract

BackgroundThe current opioid crisis has reinvigorated preclinical research in the evaluation of non-opioid candidate treatments for opioid use disorder (OUD). Emerging evidence suggests 5-HT2C receptor agonists may attenuate the abuse-related effects of opioids. This study evaluated effectiveness of 7-day treatment with the clinically available 5-HT2C agonist lorcaserin on heroin-vs.-food choice in rhesus monkeys. Lorcaserin effects were compared to effects produced by saline substitution and by 7-day treatment with the opioid antagonist naltrexone.MethodsAdult male (1) and female (6) rhesus monkeys were trained to respond under a concurrent schedule of food delivery (1g pellets, fixed-ratio 100 schedule) and intravenous heroin injections (0-0.032 mg/kg/injection, fixed-ratio 10 schedule) during daily 2h sessions. Heroin choice dose-effect functions were determined daily before and following 7-day saline substitution or 7-day continuous treatment with naltrexone (0.0032-0.032 mg/kg/h, IV) or lorcaserin (0.032-0.32 mg/kg/h, IV).ResultsUnder baseline conditions, increasing heroin doses maintained a dose-dependent increase in heroin choice. Both saline substitution and 7-day naltrexone treatment significantly attenuated heroin choice and produced a reciprocal increase in food choice. Continuous lorcaserin treatment significantly increased heroin choice.ConclusionsIn contrast to saline substitution and naltrexone, lorcaserin treatment was ineffective to reduce heroin-vs.-food choice. These preclinical results do not support the therapeutic potential of lorcaserin as a candidate OUD treatment.

Published

2019

50. Pharmacological validation of a translational model of cocaine use disorder: Effects of d-amphetamine maintenance on choice between intravenous cocaine and a nondrug alternative in humans and rhesus monkeys

Author

Katherine L. Nicholson, Abner O. Rayapati, Kevin W. Hatton, William W. Stoops, S. Stevens Negus, Justin L. Poklis, Amy R Johnson, Matthew L Banks, Craig R. Rush, Lon R. Hays, and Joshua A. Lile

Subjects

Drug, Adult, Male, Dextroamphetamine, Adolescent, media_common.quotation_subject, Self Administration, Pharmacology, Choice Behavior, Article, Cocaine-Related Disorders, Young Adult, Cocaine, Blood plasma, medicine, Potency, Animals, Humans, Pharmacology (medical), Amphetamine, media_common, business.industry, Middle Aged, medicine.disease, Macaca mulatta, Substance abuse, Psychiatry and Mental health, Cocaine use, Administration, Intravenous, Female, Self-administration, business, medicine.drug

Abstract

Drug self-administration procedures are the gold standard for laboratory research to study mechanisms of drug use disorders and evaluate candidate medications. However, preclinical-to-clinical translation has been hampered by a lack of coordination. To address this limitation, we previously developed homologous intravenous (IV) cocaine choice self-administration procedures in rhesus monkeys and humans, and then demonstrated their functional equivalence. The present studies sought to determine the sensitivity of these procedures to d-amphetamine maintenance. Three (N = 3) rhesus monkeys with histories of cocaine self-administration and 16 (N = 16) humans with cocaine use disorder completed the studies. Monkeys were maintained on IV d-amphetamine (0, 0.019, 0.037 and 0.074 mg/kg/h), and then completed 7 sessions during each condition in which they completed 9 choice trials to receive 0.14 mg/kg/injection IV cocaine (corresponding to 10 mg/70 kg in humans) or 10 food pellets under independent, concurrent progressive-ratio schedules. Humans were maintained on oral extended release d-amphetamine (0, 30 and 60 mg/day, corresponding to the lowest 3 doses in monkeys) and participated in 12 sessions in which they chose money ($6.00) or IV cocaine (0, 3, 10 and 30 mg/70 kg). Blood samples were taken to compare d-amphetamine plasma levels across species. In monkeys and humans, d-amphetamine reduced the number of cocaine choices and produced comparable blood levels at equivalent daily doses. d-Amphetamine had similar efficacy, though lower potency, at reducing choice for an equivalent cocaine dose in monkeys relative to humans. These coordinated studies support the utility of these procedures as a translational model for cocaine use disorder. (PsycInfo Database Record (c) 2020 APA, all rights reserved).

Published

2019