Please use this identifier to cite or link to this item: https://hdl.handle.net/2440/14334
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Type: Journal article
Title: Subjective and physiological responses among racemic-methadone maintenance patients in relation to relative (S)- vs. (R)-methadone exposure
Author: Mitchell, T.
Dyer, K.
Newcombe, D.
Salter, A.
Somogyi, A.
Bochner, F.
White, J.
Citation: British Journal of Clinical Pharmacology, 2004; 58(6):609-617
Publisher: Blackwell Publishing Ltd
Issue Date: 2004
ISSN: 0306-5251
1365-2125
Statement of
Responsibility: 
Timothy B. Mitchell, Kyle R. Dyer, David Newcombe, Amy Salter, Andrew A. Somogyi, Felix Bochner and Jason M. White
Abstract: AIMS: To investigate the possibility that (S)-methadone influences therapeutic and adverse responses to rac-methadone maintenance treatment, by examining how subjective and physiological responses among rac-methadone maintenance patients vary in relation to relative exposure to (S)- vs. (R)-methadone. METHODS: Mood states (Profile of Mood States), opioid withdrawal (Methadone Symptoms Checklist), physiological responses (pupil diameter, heart rate, respiration rate, blood pressure), and plasma concentrations (CP) of (R)- and (S)-methadone were measured concurrently 11–12 times over a 24-h interdosing interval in 55 methadone maintenance patients. Average steady-state plasma concentrations (Cav) and pharmacodynamic responses were calculated using area under the curve (AUC). Linear regression was used to determine whether variability in pharmacodynamic responses was accounted for by (S)-methadone Cav controlling for (R)-methadone Cav and rac-methadone dose. Ratios of (S)-:(R)-methadone using AUCCP and trough values were correlated with pharmacodynamic responses for all subjects and separately for those with daily rac-methadone doses ≥ 100 mg. RESULTS: (S)-methadone Cav accounted for significant variability in pharmacodynamic responses beyond that accounted for by (R)-methadone Cav and rac-methadone dose, showing positive associations (partial r) with the intensity of negative mood states such as Tension (0.28), Fatigue (0.31), Confusion (0.32), and opioid withdrawal scores (0.30); an opposite pattern of relationships was evident for (R)-methadone. The plasma (S)-:(R)-methadone AUCCP ratio (mean ± SD 1.05 ± 0.21, range 0.65–1.51) was not significantly related to pharmacodynamic responses for the subjects as a whole but showed significant positive associations (r) with the intensity of negative mood states such as Total Mood Disturbance (0.61), Tension (0.69), Fatigue (0.65), Confusion (0.64), Depression (0.49) and heart rate (0.59) for the ≥ 100-mg dose range. CONCLUSIONS: These findings agree with previous evidence that (S)-methadone is associated with a significant and potentially adverse profile of responses distinct from that of (R)-methadone. Individual variability in relative (S)- vs. (R)-methadone exposure may be associated with variability in response to rac-methadone maintenance treatment.
Keywords: Pupil
Humans
Opioid-Related Disorders
Substance Withdrawal Syndrome
Methadone
Narcotics
Area Under Curve
Mood Disorders
Blood Pressure
Heart Rate
Respiration
Isomerism
Adult
Middle Aged
Female
Male
Description: The definitive version is available at www.blackwell-synergy.com
DOI: 10.1111/j.1365-2125.2004.02221.x
Published version: http://dx.doi.org/10.1111/j.1365-2125.2004.02221.x
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Pharmacology publications

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