Literature DB >> 12949632

Clinical pharmacokinetics of statins.

M J García1, R F Reinoso, A Sánchez Navarro, J R Prous.   

Abstract

This article reviews the pharmacokinetic properties of HMG-CoA reductase inhibitors (or statins), as reported in humans. Most data presented here refer to commercially available statins (atorvastatin, fluvastatin, lovastatin and simvastatin), although statins that have recently been withdrawn (cerivastatin) or are currently under development (glenvastatin, pitavastatin and rosuvastatin) will also be considered. All statins with the exception of pitavastatin show very low systemic bioavailability due to an extensive first pass effect at the intestinal and/or hepatic level. Such a characteristic can be advantageous, since the liver is the target organ for statins. Unlike most statins, lovastatin and simvastatin are administered as inactive lactone prodrugs. Statins differ mainly in the degree of metabolism and the number of active and inactive metabolites. All statins but pravastatin show highly active metabolites, the pharmacological activity depending on the kinetic profile of both parent compound and active metabolites. Pravastatin has the lowest protein binding (50% vs. > 90%) and is eliminated by both metabolism and renal excretion. Atorvastatin shows the longest terminal half-life (11-14 h vs. 1-3 h). Pharmacokinetic interactions with statins are very likely to occur, particularly for those statins that are CYP3A4 substrates. However, although of extreme interest in clinical practice, this subject was extensively reviewed in a previous article and therefore is not discussed here.

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Year:  2003        PMID: 12949632

Source DB:  PubMed          Journal:  Methods Find Exp Clin Pharmacol        ISSN: 0379-0355


  25 in total

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Review 2.  Predicting the oxidative metabolism of statins: an application of the MetaSite algorithm.

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3.  Statin-associated immune-mediated necrotizing myopathy: a retrospective analysis of individual case safety reports from VigiBase.

Authors:  Dirk Essers; Martina Schäublin; Gerd A Kullak-Ublick; Stefan Weiler
Journal:  Eur J Clin Pharmacol       Date:  2018-11-15       Impact factor: 2.953

Review 4.  The effect of HMG-CoA reductase inhibitors on coenzyme Q10: possible biochemical/clinical implications.

Authors:  Iain P Hargreaves; Andrew J Duncan; Simon J R Heales; John M Land
Journal:  Drug Saf       Date:  2005       Impact factor: 5.606

Review 5.  Innovations in asthma therapy: is there a role for inhaled statins?

Authors:  Amir A Zeki; Mona Elbadawi-Sidhu
Journal:  Expert Rev Respir Med       Date:  2018-05-03       Impact factor: 3.772

6.  Personalised medicine in hypercholesterolaemia: the role of pharmacogenetics in statin therapy.

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Journal:  Ann Med       Date:  2020-08-24       Impact factor: 4.709

Review 7.  Drug-drug interactions between HMG-CoA reductase inhibitors (statins) and antiviral protease inhibitors.

Authors:  Benoit Chauvin; Sylvain Drouot; Aurélie Barrail-Tran; Anne-Marie Taburet
Journal:  Clin Pharmacokinet       Date:  2013-10       Impact factor: 6.447

8.  Effect of vitamin D on bioavailability and lipid lowering efficacy of simvastatin.

Authors:  Abdulrahman K Al-Asmari; Zabih Ullah; Fahad Al-Sabaan; Mohammad Tariq; Ahmed Al-Eid; Saud F Al-Omani
Journal:  Eur J Drug Metab Pharmacokinet       Date:  2014-04-18       Impact factor: 2.441

9.  Statin use and uterine fibroid risk in hyperlipidemia patients: a nested case-control study.

Authors:  Mostafa A Borahay; Xiao Fang; Jacques G Baillargeon; Gokhan S Kilic; Darren F Boehning; Yong-Fang Kuo
Journal:  Am J Obstet Gynecol       Date:  2016-06-28       Impact factor: 8.661

10.  Molecular Determinants of Substrate Affinity and Enzyme Activity of a Cytochrome P450BM3 Variant.

Authors:  Inacrist Geronimo; Catherine A Denning; David K Heidary; Edith C Glazer; Christina M Payne
Journal:  Biophys J       Date:  2018-08-27       Impact factor: 4.033

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