Do Formulation Differences Alter Abuse Liability of Methylphenidate?

Parasrampuria, Dolly A.; Schoedel, Kerri A.; Schuller, Regina A.; Silber, Steven A.; Ciccone, Patrick E.; Gu, Joan; Sellers, Edward M.

doi:10.1097/jcp.0b013e3181515205

Cited by 65 publications

(21 citation statements)

References 32 publications

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“…However, until a more acceptable and effective medication is available, there are few options available to clinicians to manage stimulant dependence. Extended-release formulations of agonist replacements (e.g., Concerta® or Dexedrine Spansule®) are available and should be considered until effective alternatives are identified, particularly because extended-release preparations are less likely to be misused [153, 154, 155]. …”

Section: Resultsmentioning

confidence: 99%

Agonist Replacement for Stimulant Dependence: A Review of Clinical Research

Stoops¹,

Rush²

2013

CPD

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Stimulant use disorders are an unrelenting public health concern worldwide. Agonist replacement therapy is among the most effective strategies for managing substance use disorders including nicotine and opioid dependence. The present paper reviewed clinical data from human laboratory self-administration studies and clinical trials to determine whether agonist replacement therapy is a viable strategy for managing cocaine and/or amphetamine use disorders. The extant literature suggests that agonist replacement therapy may be effective for managing stimulant use disorders, however, the clinical selection of an agonist replacement medication likely needs to be based on the pharmacological mechanism of the medication and the stimulant abused by patients. Specifically, dopamine releasers appear most effective for reducing cocaine use whereas dopamine reuptake inhibitors appear most effective for reducing amphetamine use.

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Section: Resultsmentioning

confidence: 99%

Agonist Replacement for Stimulant Dependence: A Review of Clinical Research

Stoops¹,

Rush²

2013

CPD

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“…22,39 Increasing the rate of d-MPH absorption, 32,33,58,59 and consequently the rate of delivery to the central nervous system, 19,60,61 strongly influences the stimulatory effects underlying the reward value of MPH-ethanol co-abuse. 1–10 Accordingly, the PK and psychopharmacological findings reported here provide guidance for rational drug selection and individualization when treating ADHD with or without comorbid AUD.…”

Section: Discussionmentioning

confidence: 99%

“…21,32,33 However, the 50% IR-MPH component in the SODAS formulations represents the highest IR percent of any of the several existing MR-MPH products 34 and consequently results in a PK profile closely resembling the distinct dual plasma d-MPH concentration peaks of a typical twice daily IR-MPH regimen. 35,36 …”

Section: Introductionmentioning

confidence: 99%

Ethanol Interactions With Dexmethylphenidate and dl-Methylphenidate Spheroidal Oral Drug Absorption Systems in Healthy Volunteers

Zhu

Patrick

Straughn

et al. 2017

J Clin Psychopharmacol

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Background/Purpose Ethanol co-administered with immediate-release dl-methylphenidate (dl-MPH) or dexmethylphenidate (d-MPH) significantly increases the geomean maximum plasma concentration (Cmax) of d-MPH 22% and 15%, respectively, and elevates overall drug exposure and psychostimulant effects. We asked the question: Are these ethanol-MPH interactions based more fundamentally on: (1) inhibition of post-absorption d-MPH metabolism or (2) acceleration of MPH formulation gastric dissolution by ethanol in the stomach? This was investigated using the pulsatile, distinctly biphasic, Spheroidal Oral Drug Absorption Systems of dl-MPH and d-MPH. Methods/Procedures In a randomized, 4-way crossover study, fourteen healthy subjects received pulsatile dl-MPH (40 mg) or d-MPH (20 mg), with or without ethanol (0.6 g/kg), dosed 4 hours later. These 4 hours allowed the delayed-release second MPH pulse to reach a more distal region of the gut to preclude gastric biopharmaceutical influences. Plasma was analyzed using a highly sensitive chiral method. Subjective/physiological effects were recorded. Findings/Results Ethanol increased the second pulse of d-MPH Cmax for dl-MPH by 35% (P < 0.01), and the partial area under the curve (pAUC4–8h) by 25% (P < 0.05). The respective values for enantiopure d-MPH were 27% (P = 0.001) and 20% (P < 0.01). The carboxylesterase 1-mediated transesterification metabolite ethylphenidate served as a biomarker for co-exposure. Ethanol significantly potentiated stimulant responses to either formulation. Implications/Conclusions These findings support drug dispositional interactions between ethanol and MPH as dominant over potential biopharmaceutical considerations. Understanding the pharmacology underlying the frequent co-abuse of MPH-ethanol provides rational guidance in the selection of first-line pharmacotherapy for comorbid ADHD-alcohol use disorder.

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“…Another important factor is the formulation of the medication. The reinforcing effects of stimulants are associated with rapid changes in serum concentration 39, and extended-release preparations of MPH are associated with less stimulant-like drug effects in healthy subjects 40. Of relevance to this specific psychiatric population is the fact that the OROS MPH is more difficult to use via a non-oral route (e.g.…”

Section: Discussionmentioning

confidence: 99%

Methylphenidate for attention deficit hyperactivity disorder and drug relapse in criminal offenders with substance dependence: a 24‐week randomized placebo‐controlled trial

et al. 2013

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AimTo test the efficacy and safety of osmotic release oral system (OROS) methylphenidate (MPH) in doses up to 180 mg/day to treat attention deficit hyperactivity disorder (ADHD) and prevent any drug relapse in individuals with a co-diagnosis of ADHD and amphetamine dependence.DesignRandomized placebo-controlled 24-week double-blind trial with parallel groups design.SettingParticipants were recruited from medium security prisons in Sweden. The medication started within 2 weeks before release from prison and continued in out-patient care with twice-weekly visits, including once-weekly cognitive behavioural therapy.ParticipantsFifty-four men with a mean age of 42 years, currently incarcerated, meeting DSM-IV criteria for ADHD and amphetamine dependence.MeasurementsChange in self-reported ADHD symptoms, relapse to any drug use (amphetamine and other drugs) measured by urine toxicology, retention to treatment, craving and time to relapse.FindingsThe MPH-treated group reduced their ADHD symptoms during the trial (P = 0.011) and had a significantly higher proportion of drug-negative urines compared with the placebo group (P = 0.047), including more amphetamine-negative urines (P = 0.019) and better retention to treatment (P = 0.032).ConclusionsMethylphenidate treatment reduces attention deficit hyperactivity disorder symptoms and the risk for relapse to substance use in criminal offenders with attention deficit hyperactivity disorder and substance dependence.

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Do Formulation Differences Alter Abuse Liability of Methylphenidate?

Cited by 65 publications

References 32 publications

Agonist Replacement for Stimulant Dependence: A Review of Clinical Research

Agonist Replacement for Stimulant Dependence: A Review of Clinical Research

Ethanol Interactions With Dexmethylphenidate and dl-Methylphenidate Spheroidal Oral Drug Absorption Systems in Healthy Volunteers

Methylphenidate for attention deficit hyperactivity disorder and drug relapse in criminal offenders with substance dependence: a 24‐week randomized placebo‐controlled trial

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