Literature DB >> 6749509

Clinical pharmacokinetics of atenolol--a review.

W Kirch, K G Görg.   

Abstract

Atenolol is a hydrophilic betareceptor blocking drug, which is predominantly eliminated via the kidneys, only about 5% of the atenolol is metabolised by the liver. After oral administration atenolol is incompletely absorbed from the intestine, so about 50% of the beta blocker are finally biovailable. In plasma only 3% of atenolol are protein-bound. There exists a linear relationship between the atenolol plasma levels and the degree of beta blocking effect measured by inhibition of the exercise-induced tachycardia. No correlation was found between plasma levels of atenolol and blood pressure lowering activity of the drug. After oral administration elimination half life of atenolol is calculated from 6 to 9 h by different authors. In patients with impaired renal function elimination half life of atenolol gradually increases to values of 36 h in uraemic patients (glomerular filtration rate (GFR) less than 10 ml/min). Between GFR and atenolol plasma clearance as well as renal clearance a close significant correlation is described. Prolongation of elimination half life requires a dosage adjustment of atenolol in patients with renal failure. A marked interaction of atenolol is found when calcium or aluminium hydroxide are concurrently administered with the beta blocker whereas cimetidine does not influence atenolol kinetics.

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Year:  1982        PMID: 6749509     DOI: 10.1007/BF03188723

Source DB:  PubMed          Journal:  Eur J Drug Metab Pharmacokinet        ISSN: 0378-7966            Impact factor:   2.441


  51 in total

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Journal:  Clin Pharmacol Ther       Date:  1976-05       Impact factor: 6.875

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  12 in total

1.  A cell-based molecular transport simulator for pharmacokinetic prediction and cheminformatic exploration.

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Authors:  Jose M Moltedo; Jeffrey J Kim; Richard A Friedman; Naomi J Kertesz; Bryan C Cannon
Journal:  Pediatr Cardiol       Date:  2010-10-20       Impact factor: 1.655

5.  Atenolol Renal Secretion Is Mediated by Human Organic Cation Transporter 2 and Multidrug and Toxin Extrusion Proteins.

Authors:  Jia Yin; Haichuan Duan; Yoshiyuki Shirasaka; Bhagwat Prasad; Joanne Wang
Journal:  Drug Metab Dispos       Date:  2015-09-15       Impact factor: 3.922

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7.  Improved Predictions of Drug-Drug Interactions Mediated by Time-Dependent Inhibition of CYP3A.

Authors:  Jaydeep Yadav; Ken Korzekwa; Swati Nagar
Journal:  Mol Pharm       Date:  2018-04-10       Impact factor: 4.939

8.  Functional Comparison of Human Colonic Carcinoma Cell Lines and Primary Small Intestinal Epithelial Cells for Investigations of Intestinal Drug Permeability and First-Pass Metabolism.

Authors:  Yoshiyuki Yamaura; Brian D Chapron; Zhican Wang; Jonathan Himmelfarb; Kenneth E Thummel
Journal:  Drug Metab Dispos       Date:  2015-12-23       Impact factor: 3.922

9.  Pharmacokinetic-pharmacodynamic modelling of S(-)-atenolol in rats: reduction of isoprenaline-induced tachycardia as a continuous pharmacodynamic endpoint.

Authors:  T J van Steeg; J Freijer; M Danhof; E C M de Lange
Journal:  Br J Pharmacol       Date:  2007-04-10       Impact factor: 8.739

10.  Functional identification of organic cation transporter 1 as an atenolol transporter sensitive to flavonoids.

Authors:  Yoshihisa Mimura; Tomoya Yasujima; Kinya Ohta; Katsuhisa Inoue; Hiroaki Yuasa
Journal:  Biochem Biophys Rep       Date:  2015-06-24
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