Your search keyword '"Ait-Daoud, Nassima"' showing total 10 results

1. A randomized, double-blind, placebo-controlled trial of ondansetron for the treatment of cocaine use disorder with post hoc pharmacogenetic analysis.

Author

Blevins D, Seneviratne C, Wang XQ, Johnson BA, and Ait-Daoud N

Subjects

Adult, Double-Blind Method, Humans, Ondansetron therapeutic use, Pharmacogenomic Testing, Treatment Outcome, Cocaine, Cocaine-Related Disorders drug therapy, Cocaine-Related Disorders genetics

Abstract

Background: Cocaine use disorder (CUD) has significant consequences and there remain no FDA-approved pharmacotherapies. Ondansetron is an indirect dopaminergic modulator that has shown efficacy in alcohol use disorder, particularly in phenotypic and genotypic subgroups, and was found to be efficacious in a pilot dose-finding trial for CUD., Methods: One-hundred eight (108) adults with CUD were randomized to ondansetron 4 mg twice daily or placebo for 9 weeks and assessed up to thrice weekly to evaluate self-reported cocaine use and urine benzoylecgonine. Participants received cognitive-behavioral therapy and brief behavioral compliance enhancement therapy. Consenting participants (N = 79) provided blood samples for exploratory pharmacogenetic analyses., Results: Participants in both arms reduced cocaine use over time, but there was no statistically significant difference on percentage of cocaine-free days (PCFD; p = 0.972) or percentage of cocaine-free urine samples (PCFU; p = 0.909). Participants with early-onset CUD had greater improvement regardless of study arm (p = 0.002). Post hoc pharmacogenetic analyses demonstrated an interaction effect between treatment and rs1176713 SNP on PCFU in the total sample (p = 0.040) and African ancestry subset (p = 0.03). Constipation, fatigue, and somnolence were more common among ondansetron-treated participants (Fisher exact p < 0.05). Those who developed constipation were mostly rs1176713:GG carriers (Fisher exact p = 0.029)., Conclusions: Ondansetron did not demonstrate efficacy in the treatment of CUD. However, these preliminary results suggest a genotype-based variance in response to ondansetron in African ancestry individuals with CUD. Further studies are needed to validate findings for developing a personalized genomic approach for CUD treatment in racially and ethnically diverse populations., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

2. Topiramate's effects on cocaine-induced subjective mood, craving and preference for money over drug taking.

Author

Johnson BA, Roache JD, Ait-Daoud N, Gunderson EW, Haughey HM, Wang XQ, and Liu L

Subjects

Adolescent, Adult, Affect drug effects, Cross-Over Studies, Double-Blind Method, Euphoria drug effects, Female, Fructose pharmacology, Humans, Male, Middle Aged, Patient Preference, Reinforcement, Psychology, Topiramate, Young Adult, Cocaine pharmacology, Cocaine-Related Disorders psychology, Dopamine Uptake Inhibitors pharmacology, Fructose analogs & derivatives, Neuroprotective Agents pharmacology

Abstract

Topiramate, presumably through antagonism of excitatory glutaminergic pathways and facilitation of inhibitory gamma-aminobutyric acid neurons in the cortico-mesolimbic system, might reduce cocaine's abuse liability. We tested whether topiramate (100 mg twice daily) would reduce the euphoria, subjective mood, craving and preference for cocaine over money induced by low and high doses (0.325 and 0.65 mg/kg i.v., respectively) of experimentally administered cocaine in 24 male and female, cocaine-dependent, non-treatment-seeking research volunteers in a university in-patient laboratory. We utilized a randomized, double-blind, placebo-controlled, within-subject, Latin-square cross-over design in which three experimental challenge doses of low-dose cocaine, high-dose cocaine and placebo were administered in counterbalanced order after 5 days of topiramate or matching placebo pre-treatments separated by a 1-week washout period (2006-2009). After placebo pre-treatments, cocaine produced dose-related increases in euphoria, stimulant effects, craving for more cocaine and monetary value of cocaine in a behavioral preference test of cocaine versus money choice. Topiramate pre-treatment reduced the cocaine-related craving and monetary value of high-dose cocaine while increasing the monetary value, euphoria and stimulant effects of low-dose cocaine. Validated and standardized human experimental methods evaluating the potential for topiramate to alter cocaine's abuse liability suggest that topiramate may reduce the reinforcing effects and craving induced by higher cocaine doses. Low-dose cocaine might appear to have some enhancement of its stimulant properties in the presence of topiramate's prominent sedative effects., (© 2012 The Authors, Addiction Biology © 2012 Society for the Study of Addiction.)

Published

2013

3. Effects of isradipine on cocaine-induced changes in cognitive performance in recently abstinent cocaine-dependent individuals.

Author

Johnson BA, Roache JD, Ait-Daoud N, Wallace CL, Wells LT, Wang Y, and Dawes MA

Subjects

Adult, Area Under Curve, Attention drug effects, Cocaine administration & dosage, Dose-Response Relationship, Drug, Double-Blind Method, Female, Humans, Injections, Intravenous, Male, Neuropsychological Tests, Psychiatric Status Rating Scales, Psychomotor Performance drug effects, Reaction Time drug effects, Calcium Channel Blockers pharmacology, Cocaine pharmacology, Cocaine-Related Disorders psychology, Cognition drug effects, Isradipine pharmacology

Abstract

Recently abstinent cocaine-dependent individuals, compared with healthy controls, appear more likely to exhibit deficits in cognitive performance and attention. Individuals with such cognitive deficits might be less able to avail themselves of rehabilitative or relapse-prevention efforts. Pharmacotherapy that reduces the impairment in cognitive performance among cocaine-dependent individuals would be a useful clinical tool. Preclinical and human studies suggest that the dihydropyridine-class calcium-channel antagonist, isradipine, can enhance neurocognitive function in some neuropsychiatric disorders. Isradipine, presumably by increasing cerebral blood flow and its actions at various neurotransmitter systems, might, therefore, ameliorate the impairment in cognitive performance and attention seen in cocaine addicts and enhance the expected modest improvement in performance during acute cocaine-taking in these same individuals. Among 12 male and female cocaine-dependent individuals, we examined the effects of low and high doses of intravenous cocaine (0, 0.325, and 0.650 mg/kg) on cognitive performance and attention in both the presence and absence of isradipine (0 or 30 mg sustained release each evening prior to testing, plus 0 or 15 mg immediate release each morning 2 h before the cocaine or placebo cocaine infusion and on the day of testing). Intravenous cocaine produced a modest increase in cognitive performance and attention. Isradipine, both with and without cocaine, had no effect on these same parameters. Hence, cocaine-taking by cocaine-dependent individuals produces little improvement in cognitive performance and attention in either the presence or absence of isradipine.

Published

2005

4. Effects of repeated-dose isradipine on the abuse liability of cocaine.

Author

Roache JD, Johnson BA, Ait-Daoud N, Mauldin JB, Thornton JE, Wells LT, and Murff WL

Subjects

Acetaminophen therapeutic use, Administration, Oral, Adult, Analysis of Variance, Arrhythmias, Cardiac chemically induced, Calcium Channel Blockers administration & dosage, Calcium Channel Blockers adverse effects, Cocaine-Related Disorders prevention & control, Cocaine-Related Disorders psychology, Cross-Over Studies, Delayed-Action Preparations, Dose-Response Relationship, Drug, Double-Blind Method, Emotions drug effects, Euphoria drug effects, Female, Headache chemically induced, Headache drug therapy, Heart Rate drug effects, Humans, Infusions, Intravenous, Isradipine adverse effects, Male, Middle Aged, Nausea chemically induced, Tablets, Treatment Outcome, Cocaine administration & dosage, Cocaine-Related Disorders physiopathology, Isradipine administration & dosage

Abstract

Despite preclinical studies suggesting that isradipine may antagonize the abuse liability of cocaine, pretreatment with sustained-release isradipine did not reduce euphoric mood in cocaine-using volunteers. This double-blind, within-subject, crossover laboratory study determined whether maximal dose-loading with isradipine could antagonize effects of cocaine in 12 cocaine-dependent research volunteers administered intravenous cocaine doses (0, 0.325, and 0.65 mg/kg) on different days after 5 days of treatment with isradipine or placebo. Isradipine dose was 30 mg sustained release nightly plus 15 mg immediate release 2 hr before cocaine infusion. Cocaine produced dose-related increases in cocaine's subjective effects and a behavioral measure of reinforcement. Isradipine enhanced, rather than antagonized, subjective effects, indicating that isradipine does not antagonize cocaine's abuse liability in dependent research volunteers., (Copyright 2005 APA, all rights reserved.)

Published

2005

5. Acute intravenous low- and high-dose cocaine reduces quantitative global and regional cerebral blood flow in recently abstinent subjects with cocaine use disorder.

Author

Johnson BA, Dawes MA, Roache JD, Wells LT, Ait-Daoud N, Mauldin JB, Wang Y, Lancaster JL, and Fox PT

Subjects

Adolescent, Adult, Brain drug effects, Brain pathology, Dose-Response Relationship, Drug, Female, Humans, Injections, Intravenous, Male, Middle Aged, Time Factors, Brain blood supply, Cerebrovascular Circulation drug effects, Cocaine administration & dosage, Cocaine adverse effects, Cocaine-Related Disorders physiopathology

Abstract

Cocaine-induced hypoperfusion, a risk factor for ischemic stroke, has not been fully characterized during experimental drug-taking among individuals with cocaine use disorder. We sought to examine cocaine's dose-dependent, time-related effects on cerebral blood flow. In a double-blind, randomized human laboratory study with a counterbalanced order of drug administration, 31 male and female subjects with cocaine use disorder were divided into two groups receiving either (a) low-dose cocaine (0.325 mg/kg intravenously) or placebo (N=15) or (b) high-dose cocaine (0.650 mg/kg intravenously) or placebo (N=16). The different dose conditions were administered on test days separated by a rest period of >or=48 h. Cerebral blood flow was assessed quantitatively using H(2)O(15) positron emission tomography. Experimentally administered low- and high-dose cocaine conditions versus their corresponding placebo conditions were associated with global and regional hypoperfusion. The trend for high- versus low-dose cocaine to be associated with greater hypoperfusion achieved statistical significance only for the dopamine-rich sublobar and midbrain regions. Cocaine's hypoperfusion effects were maximal at 8 mins after infusion (i.e., at about the expected peak of intravenous cocaine levels) and had mostly dissipated by 32 mins after infusion. Although hypoperfusion occurred throughout the brain, the left hemispheric dopamine-rich sublobar region was the most severely affected. Cocaine-induced cerebral hypoperfusion is associated with the time course of its pharmacological effects, and dopamine-rich areas, particularly in the left hemisphere, may be most vulnerable. Increasingly larger doses of cocaine may be associated with greater risk for ischemic stroke.

Published

2005

6. Isradipine decreases the hemodynamic response of cocaine and methamphetamine results from two human laboratory studies: results from two human laboratory studies.

Author

Johnson BA, Wells LT, Roache JD, Wallace C, Ait-Daoud N, and Wang Y

Subjects

Adult, Amphetamine-Related Disorders complications, Blood Pressure physiology, Cocaine-Related Disorders complications, Cross-Over Studies, Dose-Response Relationship, Drug, Double-Blind Method, Drug Interactions, Female, Follow-Up Studies, Humans, Hypertension chemically induced, Injections, Intravenous, Male, Stroke etiology, Stroke prevention & control, Blood Pressure drug effects, Calcium Channel Blockers therapeutic use, Cocaine adverse effects, Dopamine Uptake Inhibitors adverse effects, Heart Rate drug effects, Hypertension prevention & control, Isradipine therapeutic use, Methamphetamine adverse effects

Abstract

Background: Massive hypertensive crises relating to cerebrovascular accidents such as strokes or ruptured aneurysms, or cardiovascular dysfunction and toxicity, are an important cause of morbidity and mortality associated with cocaine or methamphetamine use. Experimentally administered, pharmacologically effective doses of cocaine and methamphetamine may serve as a model for studying the effects of these drugs on hemodynamic response and for examining the potential utility of the antihypertensive and dihydropyridine-class calcium channel antagonist isradipine to block these effects. We therefore examined, in two separate experiments of similar design conducted contemporaneously, the hemodynamic effects of cocaine or methamphetamine in the presence and absence of isradipine., Methods: In both experiments (total N = 31), isradipine pretreatment was provided to cocaine- or methamphetamine-dependent male and female subjects before intravenous administration of low and high doses of cocaine (0.325 or 0.650 mg/kg) or methamphetamine (15 or 30 mg), respectively, on separate test days., Results: Both cocaine and methamphetamine administration produced predicted elevations in blood pressure (with peak response between 1 and 3 min after infusion). Apart from tachycardia, no arrhythmias were reported. Isradipine significantly reduced stimulant-associated increases in all measures of blood pressure except pulse pressure, but tended to enhance the effects of these drugs on heart rate., Conclusions: Clinical studies are needed to determine whether isradipine is therapeutically efficacious in preventing hypertensive crises and the associated cerebrovascular and cardiovascular sequelae in cocaine- or methamphetamine-dependent individuals. As there is no established pharmacotherapy for treating cocaine or methamphetamine dependence, identification of a medication that reduces the harmful medical consequences of these drugs would be scientifically and clinically important.

Published

2005

7. Effects of isradipine on cocaine-induced subjective mood.

Author

Johnson BA, Roache JD, Ait-Daoud N, Wells LT, and Mauldin JB

Subjects

Adolescent, Adult, Area Under Curve, Calcium Channel Blockers administration & dosage, Cocaine-Related Disorders psychology, Cross-Over Studies, Dopamine metabolism, Dose-Response Relationship, Drug, Double-Blind Method, Female, Humans, Isradipine administration & dosage, Male, Reproducibility of Results, Reward, Stimulation, Chemical, Surveys and Questionnaires, Affect drug effects, Calcium Channel Blockers pharmacology, Cocaine antagonists & inhibitors, Cocaine pharmacology, Isradipine pharmacology

Abstract

We hypothesized that in humans, as in animals, isradipine, a dihydropyridine-class calcium channel antagonist, would antagonize cocaine's rewarding effects, based on preclinical evidence that isradipine inhibits cocaine-mediated increases in mesolimbic dopamine (DA), thereby reducing cocaine's abuse liability. Confirmation of our hypothesis would make isradipine a promising medication for treating cocaine dependence. Eighteen male and female volunteers (mean age, 32.6 years) who met Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition (DSM-IV) criteria for cocaine dependence participated in a double-blind, placebo-controlled, crossover study. Subjects received placebo or sustained-release (SR) low-dose or high-dose isradipine (15 or 30 mg), plus placebo or low-dose or high-dose cocaine HCl (0.325 or 0.650 mg/kg), for 9 treatment sessions separated by a 2-day interval. Standardized assessments of abuse liability, including a choice procedure to determine preference for cocaine with and without isradipine over monetary incentives, were conducted at scheduled intervals. Cocaine administration produced dose-related prototypic increases in stimulant-related effects, including euphoria, and drug preference over monetary incentives. Isradipine lacked any stimulant or abuse liability effects or the propensity to elicit craving, and it did not antagonize any of cocaine's stimulant-related effects associated with its abuse liability. In conclusion, SR isradipine (up to 30 mg) does not antagonize cocaine's rewarding effects in cocaine-dependent individuals. While higher isradipine doses may have been more effective at antagonizing cocaine reward, we could not test such doses due to the risk of serious adverse events. Also, isradipine-mediated inhibition of mesolimbic DA release may be an ineffective treatment of cocaine dependence.

Published

2004

8. TOPIRAMATE’S EFFECTS ON COCAINE-INDUCED SUBJECTIVE MOOD, CRAVING, AND PREFERENCE FOR MONEY OVER DRUG TAKING

Author

Johnson, Bankole A., Roache, John D., Ait-Daoud, Nassima, Gunderson, Erik W., Haughey, Heather M., Wang, Xin-Qun, and Liu, Lei

Subjects

Adult, Male, Cross-Over Studies, Adolescent, Patient Preference, Fructose, Euphoria, Middle Aged, Article, Affect, Cocaine-Related Disorders, Young Adult, Neuroprotective Agents, Cocaine, Dopamine Uptake Inhibitors, Double-Blind Method, Topiramate, Humans, Female, Reinforcement, Psychology

Abstract

Topiramate, presumably through antagonism of excitatory glutaminergic pathways and facilitation of inhibitory gamma-aminobutyric acid neurons in the cortico-mesolimbic system, might reduce cocaine's abuse liability. We tested whether topiramate (100 mg twice daily) would reduce the euphoria, subjective mood, craving and preference for cocaine over money induced by low and high doses (0.325 and 0.65 mg/kg i.v., respectively) of experimentally administered cocaine in 24 male and female, cocaine-dependent, non-treatment-seeking research volunteers in a university in-patient laboratory. We utilized a randomized, double-blind, placebo-controlled, within-subject, Latin-square cross-over design in which three experimental challenge doses of low-dose cocaine, high-dose cocaine and placebo were administered in counterbalanced order after 5 days of topiramate or matching placebo pre-treatments separated by a 1-week washout period (2006-2009). After placebo pre-treatments, cocaine produced dose-related increases in euphoria, stimulant effects, craving for more cocaine and monetary value of cocaine in a behavioral preference test of cocaine versus money choice. Topiramate pre-treatment reduced the cocaine-related craving and monetary value of high-dose cocaine while increasing the monetary value, euphoria and stimulant effects of low-dose cocaine. Validated and standardized human experimental methods evaluating the potential for topiramate to alter cocaine's abuse liability suggest that topiramate may reduce the reinforcing effects and craving induced by higher cocaine doses. Low-dose cocaine might appear to have some enhancement of its stimulant properties in the presence of topiramate's prominent sedative effects.

Published

2012

9. Treatment Advances for Cocaine-Induced Ischemic Stroke: Focus on Dihydropyridine-Class Calcium....

Author

Johnson, Bankole A., Devous Sr., Michael D., Ruiz, Pedro, and Ait-Daoud, Nassima

Subjects

DIHYDROPYRIDINE, CEREBRAL ischemia, COCAINE, PREVENTION

Abstract

Examines the use of dihydropyridine-class calcium channel antagonists in preventing cocaine induced cerebral ischemia. Physiological effects of cocaine abuse; Regulation of cerebral blood flow by dopamine innervated neurons; Causes of cerebral ischemia.

Published

2001

10. Kinetic and cardiovascular comparison of immediate-release isradipine and sustained-release isradipine among non-treatment-seeking, cocaine-dependent individuals

Author

Johnson, Bankole A., Javors, Martin A., Lam, Yui-Wing Francis, Wells, Lynda T., Tiouririne, Mohamed, Roache, John D., Ait-Daoud, Nassima, and Lawson, Kevin

Subjects

*CONTROLLED release drugs, *CLINICAL trials, *COCAINE, *MENTAL illness

Abstract

Abstract: The authors sought to determine whether sustained-release (SR) isradipine provided comparable systemic availability to that of immediate-release (IR) isradipine in non-treatment-seeking, cocaine-dependent individuals. This information could be used to design a rational dosage regimen for additional isradipine clinical trials in the treatment of stimulant dependence and related neurovascular disorders. Eight male volunteers who met Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition (DSM-IV) criteria for cocaine dependence participated in a randomized, double-blind, crossover study. Subjects received a 15-mg dose of an IR isradipine formulation and a 30-mg dose of an SR isradipine formulation, separated by a 2-day interval. Vital signs and blood sampling for isradipine serum levels were performed before and at 0.5, 1, 1.5, 2, 2.5, 3, 3.5, 4, 4.5, 5, 5.5, 6, 8, 10, 12, and 24 h after each isradipine dose administration. Neither the 15-mg dose of IR isradipine nor the 30-mg dose of SR isradipine produced significant adverse effects on cardiovascular parameters, but the IR formulation was more likely to produce marked short-term decreases in pressor response. Significant intersubject variability in serum concentrations and pharmacokinetic parameters occurred for both formulations. The relative bioavailability of the SR formulation was 55.5% of that of the IR formulation. Both formulations cumulatively may deliver about the same amount of drug, but IR isradipine achieves a higher peak concentration than SR isradipine. The more favorable cardiovascular profile of SR isradipine would, however, make it more appropriate as an investigational medication for the treatment of stimulant dependence and related neurovascular disorders. [Copyright &y& Elsevier]

Published

2005