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Literature DB >> 7398172

Prediction of maintenance dose required to attain a desired drug concentration at steady-state from a single determination of concentration after an initial dose.

Abstract

Strong correlations have been reported between drug concentrations at steady-state and a single drug concentration determined sometime after an initial dose for lithium, nortriptyline, imipramine, desipramine, choramphenicol and theophylline. The mathematical basis of these relationships suggests that a one point method for predicting steady-state drug concentrations and individual dosing requirements should be widely applicable to most drugs and should be valid for patients having a wide range of drug half-lives. A method is presented for evaluating the optimum time of blood sampling to determine a drug concentration in serum of plasma that best correlates with steady-state levels and for defining the range of drug half-lives beyond which the predictive approach is likely to give poor results.

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Year: 1980 PMID： 7398172 DOI： 10.2165/00003088-198005040-00005

Source DB: PubMed Journal: Clin Pharmacokinet ISSN： 0312-5963 Impact factor: 6.447

9 in total

1. The 24-hour lithium level as a prognosticator of dosage requirements: a 2-year follow-up study.

Authors: T B Cooper; G M Simpson
Journal: Am J Psychiatry Date: 1976-04 Impact factor: 18.112

2. Forecasting individual pharmacokinetics.

Authors: L B Sheiner; S Beal; B Rosenberg; V V Marathe
Journal: Clin Pharmacol Ther Date: 1979-09 Impact factor: 6.875

3. The 24-hour serum lithium level as a prognosticator of dosage requirements.

Authors: T B Cooper; P E Bergner; G M Simpson
Journal: Am J Psychiatry Date: 1973-05 Impact factor: 18.112

4. Hypothesis for the individualisation of drug dosage.

Authors: J R Koup; C M Sack; A L Smith; M Gibaldi
Journal: Clin Pharmacokinet Date: 1979 Nov-Dec Impact factor: 6.447

5. Nortriptyline in depressed patients with high plasma levels. II.

Authors: R Braithwaite; S Montgomery; S Dawling
Journal: Clin Pharmacol Ther Date: 1978-03 Impact factor: 6.875

6. A pharmacokinetic model-independent approach for estimating dose required to give desired steady-state trough concentrations of drug in plasma.

Authors: J T Slattery
Journal: J Pharmacokinet Biopharm Date: 1980-02

7. Prediction of individual dosage of nortriptyline.

Authors: T B Cooper; G M Simpson
Journal: Am J Psychiatry Date: 1978-03 Impact factor: 18.112

8. Dosage adjustment from simple nortriptyline spot level predictor tests in depressed patients.

Authors: S A Montgomery; R McAuley; D B Montgomery; R A Braithwaite; S Dawling
Journal: Clin Pharmacokinet Date: 1979 Mar-Apr Impact factor: 6.447

9. Prediction of steady-state imipramine and desmethylimipramine plasma concentrations from single-dose data.

Authors: D J Brunswick; J D Amsterdam; J Mendels; S L Stern
Journal: Clin Pharmacol Ther Date: 1979-05 Impact factor: 6.875

9 in total

21 in total

1. Poor correlation between single-dose data and steady-state kinetics for phenobarbitone, primidone, carbamazepine and sodium valproate in children during monotherapy. Possible reasons for the lack of correlation.

Authors: J A Armijo; J L Herranz; R Arteaga; R Valiente
Journal: Clin Pharmacokinet Date: 1986 Jul-Aug Impact factor: 6.447

Prediction of maintenance dose required to attain a desired drug concentration at steady-state from a single determination of concentration after an initial dose.

1. The 24-hour lithium level as a prognosticator of dosage requirements: a 2-year follow-up study.

2. Forecasting individual pharmacokinetics.

3. The 24-hour serum lithium level as a prognosticator of dosage requirements.

4. Hypothesis for the individualisation of drug dosage.

5. Nortriptyline in depressed patients with high plasma levels. II.

6. A pharmacokinetic model-independent approach for estimating dose required to give desired steady-state trough concentrations of drug in plasma.

7. Prediction of individual dosage of nortriptyline.

8. Dosage adjustment from simple nortriptyline spot level predictor tests in depressed patients.

9. Prediction of steady-state imipramine and desmethylimipramine plasma concentrations from single-dose data.

1. Poor correlation between single-dose data and steady-state kinetics for phenobarbitone, primidone, carbamazepine and sodium valproate in children during monotherapy. Possible reasons for the lack of correlation.

2. A minimax approach to the single-point method of drug dosing.

3. Simplified approaches to the determination of antipyrine pharmacokinetic parameters.

Review 4. Feedback control methods for drug dosage optimisation. Concepts, classification and clinical application.

5. Accuracy of the Pepin method to determine appropriate lithium dosages in healthy volunteers.

6. Pharmacokinetics of aspirin and salicylate in elderly subjects and in patients with alcoholic liver disease.

Review 7. Population pharmacokinetics. Theory and clinical application.

Review 8. An updated comparison of drug dosing methods. Part II: Theophylline.

9. Correlation between antithyroid effect and serum concentrations of propylthiouracil in patients with hyperthyroidism.

10. Estimating the clearance of amylobarbitone from a single plasma measurement.