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OtherBEHAVIORAL PHARMACOLOGY

Pharmacokinetic-Pharmacodynamic Modeling of Stimulatory and Sedative Effects of Alprazolam: Timing Performance Deficits

Chyan E. Lau and Anne C. Heatherington
Journal of Pharmacology and Experimental Therapeutics December 1997, 283 (3) 1119-1129;
Chyan E. Lau
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Anne C. Heatherington
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Abstract

Alprazolam decreased the reinforcement rate and increased the shorter-response rate of contingency-controlled timing behavior under a differential reinforcement of low-rate schedule (DRL 45-s) in rats. An integrated pharmacokinetic-pharmacodynamic (PK-PD) model was developed to describe and characterize the effects of i.v. and s.c. administration of alprazolam. The onset, peak and disappearance of alprazolam effects were evaluated during a 3-hr session. After s.c. alprazolam administration, two peak increases in shorter-response rate occurred at moderate alprazolam serum levels, first in the ascending and then in the descending limb of the concentration-time profile. We used a stimulation-sedation PD model incorporating two opposing effect-link sigmoidal Emax functions to model the two peaks after s.c. alprazolam administration. The model suggested that alprazolam possesses both stimulatory and sedative effects in a continuous but sequential fashion, which corresponded to low- and high-concentration effects as indicated by the EC50 values of 0.09 and 0.18 μg/ml, respectively. Owing to the rapid onset of i.v. administration, the first peak (a transition phase before the onset of the sedative effect) was absent, with the presence of the second peak again coinciding with the offset of the sedative effect. The reinforcement rate (IC50 = 0.02 μg/ml) characterized by the indirect response model to account for the initial hysteresis is an index for evaluating the deficit in timing performance. Although the effects of alprazolam can be described in behavioral terms, simultaneous PK-PD optimization numerically defines the performance and hypothesizes the coexistence of stimulation and sedation components for alprazolam. The stimulation-sedation model may help in delineating the possible mechanisms for adverse rebound side effects and of tolerance in humans.

Footnotes

  • Send reprint requests to: Chyan E. Lau, Ph.D., Department of Psychology, Busch Campus, Rutgers University, New Brunswick, NJ 08903.

  • ↵1 This research was supported by Grant R37 DA03117, awarded to J. L. Falk, from the National Institute on Drug Abuse.

  • ↵2 Supported by NIH grant NCRR RR02176.

  • ↵3 Current address: Amgen Inc., 5–1-D, 1840 DeHavilland Drive, Thousand Oaks, CA 91320.

  • Abbreviations:
    AIC
    Akaike’s Information Criterion
    BZ
    benzodiazepine
    DRL
    differential reinforcement of low rate
    EEG
    electroencephalogram
    IRT
    inter-response time
    PD
    pharmacodynamics
    PK
    pharmacokinetics
    HPLC
    high-performance liquid chromatography
    • Received December 30, 1996.
    • Accepted August 22, 1997.
  • The American Society for Pharmacology and Experimental Therapeutics
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Journal of Pharmacology and Experimental Therapeutics
Vol. 283, Issue 3
1 Dec 1997
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OtherBEHAVIORAL PHARMACOLOGY

Pharmacokinetic-Pharmacodynamic Modeling of Stimulatory and Sedative Effects of Alprazolam: Timing Performance Deficits

Chyan E. Lau and Anne C. Heatherington
Journal of Pharmacology and Experimental Therapeutics December 1, 1997, 283 (3) 1119-1129;

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OtherBEHAVIORAL PHARMACOLOGY

Pharmacokinetic-Pharmacodynamic Modeling of Stimulatory and Sedative Effects of Alprazolam: Timing Performance Deficits

Chyan E. Lau and Anne C. Heatherington
Journal of Pharmacology and Experimental Therapeutics December 1, 1997, 283 (3) 1119-1129;
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