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Consideraciones específicas en la prescripción e intercambio terapéutico de estatinas

González Juanatey, Carlos; Sempere Serrano, Paloma; García Sabina, Antonio; Gulín Dávila, Jaime; Martínez Pacheco, R
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URI: http://hdl.handle.net/20.500.11940/5042
PMID: 21820929
DOI: 10.1016/j.farma.2011.02.010
ISSN: 1130-6343
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Farma Hosp 2012;36(2):97-108 (833.9Kb)
Farm Hosp 2012;36(2):97-108 (44.20Kb)
Fecha de publicación
2012
Título de revista
Farmacia Hospitalaria
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OBJECTIVE: The pharmaceutical industry currently offers six different statins in Spain and there is one more soon to be available. Choosing the most appropriate drug and dose is determined by the therapeutic target (reduction in LDL-C levels). Statin doses that decrease LDL-C at the same percentage are considered equivalent. Evaluating the pharmacokinetic characteristics of each statin can be useful when setting selection criteria, helping to determine which statin may be more appropriate for a patient based on their individual characteristics and on the other co-administered drugs. METHODS: We reviewed the pharmacokinetics properties of each statin and its possible involvement in drug interactions. RESULTS: CYP3A4 was responsible for the metabolism of lovastatin, simvastatin and atorvastatin; fluvastatin depends on CYP2C9; P-glycoprotein is responsible for decreased atorvastatin, pravastatin, simvastatin and lovastatin concentrations. The OATPA1B1 transporter involved in all statins' access to the hepatocyte, except for fluvastatin, is essential for rosuvastatin and pravastatin. These circumstances cause those drugs inhibiting or inducing isoenzymes or transporters' activity not to have the same effect on the different statins. CONCLUSION: The pharmacokinetics is important when choosing the best statin and could be a limitation in the use of interchange therapeutic programmes when other drugs are present.

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