Simultaneous modeling of pharmacokinetics and pharmacodynamics: Application to <i>d</i>‐tubocurarine

Sheiner, Lewis B.; Stanski, Donald R.; Vozeh, S; Miller, Ronald D.; Ham, Jay

doi:10.1002/cpt1979253358

Cited by 1,064 publications

(551 citation statements)

References 5 publications

(6 reference statements)

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“…PK and PKPD analysis was achieved by use of the compartmental modeling SAAM II software system (SAAM Institute, Seattle, WA, USA). A link compartment representing stimulation of the locomotor behavior was used to describe the data (Sheiner et al 1979). Integration of mephedrone pharmacokinetics and pharmacodynamics was based on the relationship between mean plasma mephedrone concentration-time profile for i.v.…”

Section: Locomotor Activity Experimentsmentioning

confidence: 99%

Mephedrone pharmacokinetics after intravenous and oral administration in rats: relation to pharmacodynamics

et al. 2013

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Rationale Mephedrone (4-methylmethcathinone) is a still poorly known drug of abuse, alternative to ecstasy or cocaine.Objective The major aims were to investigate the pharmacokinetics and locomotor activity of mephedrone in rats and provide a pharmacokinetic/pharmacodynamic model. MethodsMephedrone was administered to male Sprague-Dawley rats intravenously (10 mg/kg) and orally (30 and 60 mg/kg). Plasma concentrations and metabolites were characterized by LC/MS and LC-MS/MS fragmentation patterns. Locomotor activity was monitored for 180-240 min.Results Mephedrone plasma concentrations after i.v. administration fit to a twocompartment model (α=10.23 h -1 and β=1.86 h -1 ). After oral administration, peak mephedrone concentrations were achieved between 0.5-1 h, and declined to undetectable levels at 9 h. Absolute bioavailability of mephedrone was of about 10% and the percentage of mephedrone protein binding was of 21.59 ± 3.67%. We have identified five Phase I metabolites in rat blood after oral administration. The relationship between brain levels and free plasma concentration was 1.85 ± 0.08.Mephedrone induced a dose-dependent increase in locomotor activity, which lasted up to 2 h. The pharmacokinetic-pharmacodynamic model successfully describes the relationship between mephedrone plasma concentrations and its psychostimulant effect. ConclusionsWe suggest a very important first-pass effect for mephedrone after oral administration and an easy access to the central nervous system. The model described might be useful in the estimation and prediction of the onset, magnitude and time course of mephedrone pharmacodynamics as well as to design new animal models of mephedrone addiction and toxicity.

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Section: Locomotor Activity Experimentsmentioning

confidence: 99%

Mephedrone pharmacokinetics after intravenous and oral administration in rats: relation to pharmacodynamics

et al. 2013

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“…A link compartment representing stimulation of the locomotor behavior was used to describe the data (Sheiner et al, 1979). Integration of methylone pharmacokinetics and pharmacodynamics was based on the relationship between mean plasma methylone concentration-time profile for i.v.…”

Section: Pharmacokinetic/pharmacodynamics Analysismentioning

confidence: 99%

“…This hysteresis can be explained by the appearance of active metabolites (Mandema et al, 1992); by indirect mechanisms of drug action (Dayneka et al, 1993) or by an imbalance between the site of action (the brain) and the plasmatic compartment (Sheiner et al, 1979).…”

Section: Accepted M Manuscriptmentioning

confidence: 99%

An integrated pharmacokinetic and pharmacodynamic study of a new drug of abuse, methylone, a synthetic cathinone sold as “bath salts”

López-Arnau

Martínez-Clemente

Carbó

et al. 2013

Progress in Neuro-Psychopharmacology and Biological Psychiatry

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“…Plasma concentrations of the parent drug and of its metabolite Perindopril and perindoprilat plasma concentrations (ng ml x1 ) were determined from venous blood samples by radioimmunoassay as previously described [20]. Measurements were performed before and 0.5, 1, 1.5, 2, 2.5, 3,4,6,8,10,12,16,20,24,48 and 72 h after drug intake in HV. In CHF patients, the same schedule was used except that the two samples drawn at 16 and 20 h were replaced by a single one drawn at 18 h. The detection limit of the assay was 0.4 ng ml x1 for both perindopril and perindoprilat.…”

Section: Experimental Protocolmentioning

confidence: 99%

Pharmacokinetic–pharmacodynamic model for perindoprilat regional haemodynamic effects in healthy volunteers and in congestive heart failure patients

Giudicelli

2001

Brit J Clinical Pharma

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Aims We compared the relationships between the plasma concentrations (C) of perindoprilat, active metabolite of the angiotensin I-converting enzyme inhibitor (ACEI) perindopril, and the effects (E) induced on plasma converting enzyme activity (PCEA) and brachial vascular resistance (BVR) in healthy volunteers (HV) and in congestive heart failure (CHF) patients after single oral doses of perindopril. Methods Six HV received three doses of perindopril (4, 8, 16 mg) in a placebocontrolled, randomized, double-blind, crossover study whereas 10 CHF patients received one dose (4 mg) in an open study. Each variable was determined before and 6±12 times after drug intake. E (% variations from baseline) were individually related to C (ng ml x1 ) by the Hill model E=E max .C c /(CE 50 c +C c ). When data showed a hysteresis loop, an effect compartment was used. Results (meansts.d.) In HV, relationships between C and E were direct whereas in CHF patients, they showed hysteresis loops with optimal k e0 values of 0.13t0.16 and 0.13t0.07 h x1 for PCEA and BVR, respectively. For PCEA, with E max set to x100%, CE 50 =1.87t0.60 and 1.36t1.33 ng ml x1 (P=0.34) and c =0.90t0.13 and 1.11t0.47 (P=0.23) in HV and CHF patients, respectively. For BVR, E max = x41t14% and x60t7% (P=0.02), CE 50 =4.95t2.62 and 1.38t0.85 ng ml x1 (P=0.02), and c =2.25t1.54 and 3.06t1.37 (P=0.32) in HV and CHF patients, respectively. Conclusions Whereas concentration-effect relationships were similar in HV and CHF patients for PCEA blockade, they strongly differed for regional haemodynamics. This result probably expresses the different involvements, in HV and CHF patients, of angiotensinergic and nonangiotensinergic mechanisms in the haemodynamic effects of ACEIs.

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Simultaneous modeling of pharmacokinetics and pharmacodynamics: Application to d‐tubocurarine

Cited by 1,064 publications

References 5 publications

Mephedrone pharmacokinetics after intravenous and oral administration in rats: relation to pharmacodynamics

Mephedrone pharmacokinetics after intravenous and oral administration in rats: relation to pharmacodynamics

An integrated pharmacokinetic and pharmacodynamic study of a new drug of abuse, methylone, a synthetic cathinone sold as “bath salts”

Pharmacokinetic–pharmacodynamic model for perindoprilat regional haemodynamic effects in healthy volunteers and in congestive heart failure patients

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