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Vol. 16. Núm. 6.
Páginas 227-232 (Enero 2004)
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Vol. 16. Núm. 6.
Páginas 227-232 (Enero 2004)
DOI: 10.1016/S0214-9168(04)78998-6
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Efecto de diferentes polimorfismos en el gen del OATP-C sobre la respuesta hipolipemiante al tratamiento con pravastatina
Effect of different polymorphisms in OATP-C gene on the hypolipidemic response to pravastatin therapy
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R. Peñaa, J.M. Mostazaa,
Autor para correspondencia
jmostaza.hciii@salud.madrid.org

Correspondencia: Unidad de Arteriosclerosis. Hospital Carlos III. Sinesio Delgado, 10. 28029 Madrid. España
, C. Lahoza, E. Subiratsb, X. Pintóc, F. Lagunaa, M.F. García-Iglesiasa, E. Torrecillaa
a Unidad de Arteriosclerosis. Hospital Carlos III. Madrid. España
b Servicio de Medicina Interna. Hospital de Puigcerdà. Puigcerdà. Girona. España
c Unidad de lípidos. Hospital de Bellvitge. L’Hospitalet de Llobregat. Barcelona. España
grupo del estudio RAP
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Fundamento

Existe una gran variabilidad en la respuesta de los lípidos y lipoproteínas plasmáticas al tratamiento con estatinas, en parte debida a factores genéticos. Recientemente se han identificado diversos polimorfismos en el gen del OATP-C, transportador implicado en la internalización de la pravastatina en el hepatocito, que afectan a su actividad. El objetivo del presente estudio fue evaluar el efecto de diferentes polimorfismos en el gen del OATP-C sobre la respuesta de los lípidos y las lipoproteínas plasmáticas a la pravastatina

Pacientes y métodos

Se seleccionó a 290 sujetos hipercolesterolémicos (el 56% mujeres, con una edad media de 57 años), con indicación de tratamiento farmacológico hipolipemiante tras seguir una dieta baja en grasa saturada y colesterol. Las determinaciones de lípidos y lipoproteínas se realizaron de forma centralizada, antes y después de 16 semanas de tratamiento, con 20 mg/día de pravastatina

Resultados

El polimorfismo T217C en el exón 2 del gen del OATP-C no se detectó en ningún sujeto de nuestra población. La distribución del polimorfismo T521C en el exón 5 fue de un 70% el T/T, 29% el T/C y 1% el C/C. El polimorfismo T521C no tuvo ningún efecto sobre los valores basales de lípidos ni sobre su respuesta al tratamiento con pravastatina

Conclusión

El polimorfismo T521C en el exón 5 del gen del OATP-C no influye sobre la respuesta hipolipemiante a la pravastatina

Palabras clave:
Polimorfismos genéticos
OATP-C
Pravastatina
Colesterol
Background

Considerable variability exists in the plasma lipid and lipoprotein response to statin treatment due, in part, to genetic factors. Multiple polymorphisms in the OATP-C gene, a transporter involved in the hepatic uptake of pravastatin, some of which affect the transport activity, have recently been identifed. The aim of the present study was to evaluate the effect of different polymorphisms in the OATP-C gene on the plasma lipoprotein response to pravastatin treatment

Patients and methods

290 subjects (56% women; mean age: 57 years) who were hypercholesterolemic despite a diet poor in saturated fat and cholesterol were selected for this study. Plasma lipids and lipoproteins were measured centrally, before and after 16 weeks of treatment with 20 mg/d of pravastatin

Results

The T217C polymorphism in exon 2 of the OATP-C gene was not detected in our population. Distribution of the T521C polymorphism in exon 5 was 70% T/T, 29% T/C and 1% C/C. The T521C polymorphism neither influenced baseline lipid and lipoprotein levels nor their response to pravastatin therapy

Conclusion

The T521C polymorphism in exon 5 of the OATP-C gene does not appear to influence the hypolipidemic effect of pravastatin treatment

Key words:
Genetic polymorphisms
OATP-C
Pravastatin
Cholesterol
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Bibliografía
[1.]
The long-term intervention with pravastatin in ischaemic disease (LIPID) study group. prevention of cardiovascular events and death with pravastatin in patients with coronary heart disease and a broad range of initial cholesterol levels.
N engl j med, 339 (1998), pp. 1349-1357
http://dx.doi.org/10.1056/NEJM199811053391902 | Medline
[2.]
F.M. Sacks, M.A. Pfeffer, L.A. Moye, J.L. Rouleau, J.D. Rutherford, T.G. Cole, et al.
The effect of pravastatin on coronary events after myocardial infarction in patients with average cholesterol levels. cholesterol and recurrent events trial investigators.
N engl j med, 335 (1996), pp. 1001-1009
http://dx.doi.org/10.1056/NEJM199610033351401 | Medline
[3.]
J. Shepherd, S.M. Cobbe, I. Ford, C.G. Isles, A.R. Lorimer, P.W. MacFarlane, et al.
Prevention of coronary heart disease with pravastatin in men with hypercholesterolemia. west of scotland coronary prevention study group.
N engl j med, 333 (1995), pp. 1301-1307
http://dx.doi.org/10.1056/NEJM199511163332001 | Medline
[4.]
Influence of pravastatin and plasma lipids on clinical events in the west of scotland coronary prevention study (WOSCOPS).
Circulation, 97 (1998), pp. 1440-1445
Medline
[5.]
J. Pedro-Botet, E.J. Schaefer, R.G. Bakker-Arkema, D.M. Black, E.M. Stein, D. Corella, et al.
Apolipoprotein e genotype affects plasma lipid response to atorvastatin in a gender specific manner.
Atherosclerosis, 158 (2001), pp. 183-193
Medline
[6.]
K. Nakajima.
Sex-related differences in response of plasma lipids to simvastatin: the saitama postmenopausal lipid intervention study.S-POLIS group.
Clin ther, 21 (1999), pp. 2047-2057
Medline
[7.]
M.M. Cobb, H.S. Teitelbaum, J.L. Breslow.
Lovastatin efficacy in reducing low-density lipoprotein cholesterol levels on high- versus low-fat diets.
JAMA, 265 (1991), pp. 997-1001
Medline
[8.]
A.R. Miserez, F.A. Rossi, U. Keller.
Prediction of the therapeutic response to simvastatin by pretreatment lipid concentrations in 2.082 subjects.
Eur j clin pharmacol, 46 (1994), pp. 107-114
Medline
[9.]
S. Drmanac, D.C. Heilbron, C.R. Pullinger, M. Jafari, D. Gietzen, T. Ukrainczyk, et al.
Elevated baseline triglyceride levels modulate effects of HMGCoA reductase inhibitors on plasma lipoproteins.
J cardiovasc pharmacol ther, 6 (2001), pp. 47-56
Medline
[10.]
J.M. Ordovas, J. López-Miranda, F. Pérez-Jiménez, C. Rodríguez, J.S. Park, T. Cole, et al.
Effect of apolipoprotein E and A-IV phenotypes on the low density lipoprotein response to HMG CoA reductase inhibitor therapy.
Atherosclerosis, 113 (1995), pp. 157-166
Medline
[11.]
C. Lahoz, R. Peña, J.M. Mostaza, J. Jiménez, E. Subirats, X. Pinto, et al.
Apo A-I promoter polymorphism influences basal HDL-cholesterol and its response to pravastatin therapy.
Atherosclerosis, 168 (2003), pp. 289-295
Medline
[12.]
E. Leitersdorf, S. Eisenberg, O. Eliav, Y. Friedlander, N. Berkman, E.J. Dann, et al.
Genetic determinants of responsiveness to the HMG-CoA reductase inhibitor fluvastatin in patients with molecularly defined heterozygous familial hypercholesterolemia.
Circulation, 87 (1993), pp. III35-III44
Medline
[13.]
A. Zambon, S.S. Deeb, B.G. Brown, J.E. Hokanson, J.D. Brunzell.
Common hepatic lipase gene promoter variant determines clinical response to intensive lipid-lowering treatment.
Circulation, 103 (2001), pp. 792-798
Medline
[14.]
J.W. Jukema, A.J. Van Boven, B. Groenemeijer, A.H. Zwinderman, J.H. Reiber, A.V. Bruschke, et al.
The asp9asn mutation in the lipoprotein lipase gene is associated with increased progression of coronary atherosclerosis. REGRESS. (regression growth evaluation statin study).
Circulation, 94 (1996), pp. 1913-1918
Medline
[15.]
A. Corsini, M. Mazzotti, R. Fumagalli, A.L. Catapano, L. Romano, C. Romano.
Poor response to simvastatin in familial defective apo-B- 100 [carta].
Lancet, 337 (1991), pp. 305
Medline
[16.]
M. Jeenah, W. September, F. Graadt van Roggen, W. De Villiers, H. Seftel, D. Marais.
Influence of specific mutations at the LDL-receptor gene locus on the response to simvastatin therapy in Afrikaner patients with heterozygous familial hypercholesterolaemia.
Atherosclerosis, 98 (1993), pp. 51-58
Medline
[17.]
C.M. Ballantyne, J.A. Herd, E.A. Stein, L.L. Ferlic, J.K. Dunn, A.M. Gotto, et al.
Apolipoprotein e genotypes and response of plasma lipids and progression-regression of coronary atherosclerosis to lipid-lowering drug therapy.
J am coll cardiol, 36 (2000), pp. 1572-1578
Medline
[18.]
A.C. Nestruck, D. Bouthillier, C.F. Sing, J. Davignon.
Apolipoprotein e polymorphism and plasma cholesterol response to probucol.
Metabolism, 36 (1987), pp. 743-747
Medline
[19.]
M. Eto, T. Sato, K. Watanabe, Y. Iwashima, I. Makino.
Effects of probucol on plasma lipids and lipoproteins in familial hypercholesterolemic patients with and without apolipoprotein e4.
Atherosclerosis, 84 (1990), pp. 49-53
Medline
[20.]
T. Abe, M. Kakyo, T. Tokui, R. Nakagomi, T. Nishio, D. Nakai, et al.
Identification of a novel gene family encoding human liver-specific organic anion transporter LST-1.
J biol chem, 274 (1999), pp. 17159-17163
Medline
[21.]
B. Hsiang, Y. Zhu, Z. Wang, Y. Wu, V. Sasseville, W.P. Yang, et al.
A novel human hepatic organic anion transporting polypeptide (OATP2). Identification of a liver-specific human organic anion transporting polypeptide and identification of rat and human hydroxymethylglutaryl- CoA reductase inhibitor transporters.
J biol chem, 274 (1999), pp. 37161-37168
Medline
[22.]
D. Nakai, R. Nakagomi, Y. Furuta, T. Tokui, T. Abe, T. Ikeda, et al.
Human liver-specific organic anion transporter, LST-1, mediates uptake of pravastatin by human hepatocytes.
J pharmacol exp ther, 297 (2001), pp. 861-867
Medline
[23.]
D. Jung, B. Hagenbuch, L. Gresh, M. Pontoglio, P.J. Meier, G.A. Kullak-Ublick.
Characterization of the human OATP-C (SLC21A6) gene promoter and regulation of liver-specific OATP genes by hepatocyte nuclear factor 1 alpha.
J biol chem, 276 (2001), pp. 37206-37214
http://dx.doi.org/10.1074/jbc.M103988200 | Medline
[24.]
R.G. Tirona, B.F. Leake, G. Merino, R.B. Kim.
Polymorphisms in OATP-C: identification of multiple allelic variants associated with altered transport activity among european- and african-americans.
J biol chem, 276 (2001), pp. 35669-35675
http://dx.doi.org/10.1074/jbc.M103792200 | Medline
[25.]
T. Nozawa, M. Nakajima, I. Tamai, K. Noda, J. Nezu, Y. Sai, et al.
Genetic polymorphisms of human organic anion transporters OATPC (SLC21A6) and OATP-B (SLC21A9): allele frequencies in the Japanese population and functional analysis.
J pharmacol exp ther, 302 (2002), pp. 804-813
Medline
[26.]
W.T. Friedewald, R.I. Levy, D.S. Fredrickson.
Estimation of the concentration of low-density lipoprotein cholesterol in plasma, without use of the preparative ultracentrifuge.
Clin chem, 18 (1972), pp. 499-502
Medline
[27.]
W. Kalow, B.K. Tang, L. Endrenyi.
Hypothesis: comparisons of inter- and intra-individual variations can substitute for twin studies in drug research.
Pharmacogenetics, 8 (1998), pp. 283-289
Medline
[28]
R. Sachidanandam, D. Weissman, S.C. Schmidt, J.M. Kakol, L.D. Stein, G. Marth, et al.
A map of human genome sequence variation containing 1.42 million single nucleotide polymorphisms.
Nature, 409 (2001), pp. 928-933
http://dx.doi.org/10.1038/35057149 | Medline
[29.]
W.E. Evans, M.V. Relling.
Pharmacogenomics: translating functional genomics into rational therapeutics.
Science, 286 (1999), pp. 487-491
Medline
[30.]
U.A. Meyer, U.M. Zanger.
Molecular mechanisms of genetic polymorphisms of drug metabolism.
Annu rev pharmacol toxicol, 37 (1997), pp. 269-296
http://dx.doi.org/10.1146/annurev.pharmtox.37.1.269 | Medline
[31.]
C.F. Sing, J. Davignon.
Role of the apolipoprotein e polymorphism in determining normal plasma lipid and lipoprotein variation.
Am j hum genet, 37 (1985), pp. 268-285
Medline
[32.]
C. Michalski, Y. Cui, A.T. Nies, A.K. Nuessler, P. Neuhaus, U.M. Zanger, et al.
A naturally occurring mutation in the SLC21A6 gene causing impaired membrane localization of the hepatocyte uptake transporter.
J biol chem, 277 (2002), pp. 43058-43063
http://dx.doi.org/10.1074/jbc.M207735200 | Medline
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