A propranolol radioimmunoassay and its use in the study of its pharmaco‐kinetics following low doses

Mould, G P; Clough, Jacqueline M.; Morris, B.; Stout, G.; Marks, Vincent

doi:10.1002/bdd.2510020106

Cited by 17 publications

(11 citation statements)

References 10 publications

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“…This argument can be further verified by comparison of the mean observed clearance (CL) 0.82 L/h/kg (95% CI: 0.64-1.00) [26][27][28]46,47 with mean predicted clearance 0.99 L/h/kg (95% CI: 0.70-1.2) after IV administration. Similarly, CL/F in healthy individuals was also comparable, as its observed and reported values were 217 L/h (95% CI: 183.6-250.80) 26,[29][30][31][32][33]46,[48][49][50][51][52] and 183.3 L/h (95% CI: 169.9-196.6), respectively. Furthermore, the AFE value for CL (0.83 and 1.15 after IV and oral dose predictions) strengthened the argument that the developed PBPK model was predicting the disposition of the drug precisely (Table 4).…”

Section: Discussionsupporting

confidence: 73%

“…Data from 22 clinical studies (7 for IV administration and 15 for oral administration) in healthy individuals was extracted. One-third (3 IV 26-28 and 5 oral [29][30][31][32][33] ) of which were used for the development of the PBPK model and the rest of the two-thirds (4 IV and 10 oral) were used for subsequent model verifications. All the observed data sets were used for model evaluation.…”

Section: Materials and Methodology Clinical Pharmacokinetic Datamentioning

confidence: 99%

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Development and Evaluation of a Physiologically Based Pharmacokinetic Drug-Disease Model of Propranolol for Suggesting Model Informed Dosing in Liver Cirrhosis Patients

Kalam¹,

Rasool²,

Alqahtani³

et al. 2021

DDDT

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The study was aimed to understand the underlying causes for the differences in propranolol pharmacokinetics (PK) between healthy and cirrhosis populations by using a systematic whole-body physiologically based pharmacokinetic (PBPK) model-building approach for suggesting model informed propranolol dosing in liver cirrhosis patients with different stages of disease severity. Methods: A whole-body PBPK model was developed by using population simulator PK-Sim ® by using reported physicochemical and clinical data for propranolol in healthy and liver cirrhosis populations. The model evaluation was done by visual verification and comparison of PK parameters using their observed/predicted ratios (R obs/pred). Results: The developed model has effectively described the disposition of propranolol after intravenous and oral application in healthy and liver cirrhosis populations. All the model predictions were comparable to the observed clinical data and the R obs/pred for all the PK parameters were within a 2-fold range. A significant increase in plasma concentration of propranolol and decrease in drug clearance was observed in progressive stages of liver cirrhosis. The developed model after evaluation with the reported clinical PK data was used for suggesting model informed propranolol dosing in different stages of liver cirrhosis based on systemic unbound drug concentration. Conclusion: The developed PBPK model has successfully described propranolol PK in healthy and cirrhosis populations after IV and oral administration. The evaluated PBPK propranolol-cirrhosis model can have many implications in predicting propranolol dosing in liver cirrhosis patients with different stages of disease severity.

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Section: Discussionsupporting

confidence: 73%

Section: Materials and Methodology Clinical Pharmacokinetic Datamentioning

confidence: 99%

Development and Evaluation of a Physiologically Based Pharmacokinetic Drug-Disease Model of Propranolol for Suggesting Model Informed Dosing in Liver Cirrhosis Patients

Kalam¹,

Rasool²,

Alqahtani³

et al. 2021

DDDT

View full text Add to dashboard Cite

show abstract

“…Although it has been shown that the liver metabolism is non-linear, saturating at high blood levels, this non-linearity only becomes significant at doses above 200 mg/day [35]. At lower doses, both the liver metabolism and PO absorption appear to be linear [36,37]. All the data that will be used here fall in this linear dose range.…”

Section: Resultsmentioning

confidence: 99%

PKQuest: a general physiologically based pharmacokinetic model. Introduction and application to propranolol

Levitt¹

2002

BMC Clin Pharmacol

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“…The plasma samples were assayed in duplicate using the specific radioimmunoassay for propranolol previously developed (9). Although the sensitivity of the assay is 2 .…”

Section: Assay Of Plasma Samplesmentioning

confidence: 99%

“…A recently developed radioimmunoassay technique (9) has enabled propranolol to be measured following low doses of drug, allowing subjects to take significantly less proprano-lo1 than in previous studies (8,10). Accordmgly the plasma concentration profiles following 10 mg propranolol hydrochloride from two different tablets and a freshly prepared solution were compared.…”

Section: Introductionmentioning

confidence: 99%

A Bioequivalence Study of Three Preparations of Propranolol

Mould

Clough

Levinson³

et al. 1982

J Clin Pharm Ther

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SUMMARY The bioequivalence of two different tablets and a solution, each containing 10 mg propranolol hydrochloride was studied in twelve healthy volunteers. Single oral doses of each preparation were administered at intervals of one week. Samples of blood for propranolol radioimmunoassay were taken up to 8 h after dosing. The plasma propranolol concentration at 0.5 h was significantly higher for the solution than for the two tablet formulations which did not differ significantly from each other at any sampling point. The area under the curve was similar for all three preparations. The study demonstrated that the three different preparations of propranolol were bioequivalent.

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A propranolol radioimmunoassay and its use in the study of its pharmaco‐kinetics following low doses

Cited by 17 publications

References 10 publications

Development and Evaluation of a Physiologically Based Pharmacokinetic Drug-Disease Model of Propranolol for Suggesting Model Informed Dosing in Liver Cirrhosis Patients

Development and Evaluation of a Physiologically Based Pharmacokinetic Drug-Disease Model of Propranolol for Suggesting Model Informed Dosing in Liver Cirrhosis Patients

PKQuest: a general physiologically based pharmacokinetic model. Introduction and application to propranolol

A Bioequivalence Study of Three Preparations of Propranolol

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