High baseline serum total and LDL cholesterol levels are associated with MDR1 haplotypes in Brazilian hypercholesterolemic individuals of European descent

Rodrigues, Alice Cristina; Rebecchi, Ivanise Marina Moretti; Bertolami, Marcelo Chiara; Faludi, André Árpád; Hirata, Mário Hiroyuki; Hirata, Rosário Dominguez Crespo

doi:10.1590/s0100-879x2005000900014

Cited by 55 publications

(46 citation statements)

References 37 publications

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“…The results are similar to the frequencies observed by Wielandt et al (2004) in Mapuche and Mestizo ethnicities of our country, having allelic frequencies of 0.35 and 0.33, respectively. Similarly, in Brazilian hypercholesterolemic subjects, the frequency was 0.47 for T allele (Rodrigues et al, 2005). In addition, the frequency found in our study, for the T allele of the variant 3435C> T is similar to that observed in Asian population such as Koreans (0.37) (Yi et al, 2004), higher in Rapanui populations (0.75) (Wielandt et al), and differs significantly from that observed in Afro-Americans (0.21) (Kajinami et al, 2004b), Africans (0.17), European Caucasian (0.52) (Ameyaw et al, 2001) and Oceania population (0.53) (Roberts et al, 2002).…”

Section: Discussionmentioning

confidence: 88%

“…This includes genes relevant to metabolizing enzymes such a CYP3A4 and CYP3A5 gene (Lee et al, 2002), transport protein MDR1 (ABCB1) gene (Ayrton & Morgan, 2001), cholesterol biosynthesis (HMGCR). In these studies, different common variants were identified -260A>G (CYP3A4) (Kajinami et al, 2004a), 6986A>G (CYP3A5) (Kim et al, 2007) and 3435C>T (ABCB1 or MDR1) (Rodrigues et al, 2005) which were associated to a possible response variation and with efficacy of lipid-lowering therapy. CYP3A5*3 allele, was found to cause alternative splicing and protein truncation, resulting in the absence of functional CYP3A5 from liver tissue (Kuehl et al, 2001).…”

Section: Introductionmentioning

confidence: 99%

“…The integrity of the genomic DNA was evaluated by electrophoresis in a 1.5% agarose gel. The 3535C>T (ABCB1), -290A>G (CYP3A4) and 6986A>G (CYP3A5) gene polymorphisms were detected using polymerase chain reaction followed by restriction fragment length polymorphism (PCR-RFLP) in according to conditions previously described (Cavalli et al, 2001;Rodrigues et al, 2005;Kim et al). As positive control a homozygous sample for each variant was included.…”

Section: Introductionmentioning

confidence: 99%

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Frequency of Common Variants in Genes Involved in Lipid-Lowering Response to Statins in Chilean Subjects with Hypercholesterolemia

et al. 2011

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SUMMARY: Interindividual differences in activity and expression of the metabolizing enzymes cytochrome P450 (CYP) 3A4 and 3A5 and the multidrug efflux pump P-glycoprotein (P-gp, encoded by ABCB1 gene) contribute considerably to lipid-lowering efficacy of statin treatment in subjects with hypercholesterolemia. Variability in the activity of CYP3A4, CYP3A5 and P-gp could be considered to result from genetic polymorphisms encoding their genes. However, the available data indicate that the frequencies of ABCB1, CYP3A4 and CYP3A5 gene polymorphisms differ significantly across populations. Thus, the aim of the present study was to determine the allelic frequency of three common variants of these genes in Chilean individuals with primary hypercholesterolemia (HC) and controls. A total of 135 unrelated patients (44 ± 7 years old) with diagnosis of hypercholesterolemia (Total cholesterol ≥ 240 mg/dL) and 120 normolipidemic healthy controls (40 ± 10 years old; total cholesterol ≤ 200 mg/dL) were included in this study. The 3435C>T (MDR1), -290A>G (CYP3A4) and 6986A>G (CYP3A5) gene polymorphisms were analyzed by PCR-RFLP. The genotype distribution for 3435C>T variant of ABCB1 in HC patients (CC: 49%, CT: 37%, TT: 14%) and controls (CC: 41%, CT: 48%, TT: 11%) was comparable (P=0.186). Similarly, the genotype distribution for -290A>G polymorphism of CYP3A4 in HC subjects (AA: 73%, AG: 27%, GG: 0%) and controls (AA: 71%, AG: 29%, GG: 0%) was equivalent (P = 0.863). Finally, the genotype distribution for 6986A>G variant of CYP3A5 in HC individuals (AA: 4%, AG: 41%, GG: 55%) and controls (AA: 4%, AG: 47%, GG: 49%) was similar (P=0.594). The allelic frequencies of 3435C>T (ABCB1), -290A>G (CYP3A4) and 6986A>G (CYP3A5) polymorphisms are similar between Chilean HC patients and controls, and comparable to frequencies found in Asian populations.

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Section: Discussionmentioning

confidence: 88%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Frequency of Common Variants in Genes Involved in Lipid-Lowering Response to Statins in Chilean Subjects with Hypercholesterolemia

et al. 2011

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“…For example, in a study from USA, common variants of MDR1 gene such as the C3435T, were associated with a smaller reduction in LDL and with a larger increase in HDL levels, relative to variant allele carriers (Kajinami et al 2004). However, other studies among Brazilian of European descents and USA populations, found no significant relation between atorvastatin response and MDR1 C3435T polymorphism (Mega et al 2009;Rodrigues et al 2005). In the current study, we examined the influence of three common MDR1 gene variants on lipid response to atorvastatin treatment among Jordanians.…”

Section: Introductionmentioning

confidence: 95%

The role of Multidrug Resistance-1 (MDR1) variants in response to atorvastatin among Jordanians

et al. 2014

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The MDR1 gene encodes for P-glycoprotein (P-gp), which is an efflux transporter at the cell membrane. The P-gp has wide substrate specificity for multiple medications including the lipid lowering drug, atorvastatin. In this study, we investigated the possible association between three common MDR1 gene polymorphisms (G2677T, C3435T, and C1236T), and the lipid lowering effect of atorvastatin among Jordanians. Lipid and lipoproteins were measured in blood samples collected from patients (n = 201) at baseline and during atorvastatin treatment. MDR1 polymorphisms were genotyped using polymerase chain reaction-restriction fragment length polymorphism. Both the TT genotype of G2677T and the TT genotype of the C3435T polymorphisms were associated with lower levels of low-density lipoproteins after atorvastatin treatment. However, the effects of atorvastatin on the levels of total cholesterol, triglycerides, and high-density lipoprotein, were not correlated with any of the genotypes in both polymorphisms. Finally, the C1236T polymorphism was not associated with the lipid lowering effect of atorvastatin. In conclusion, the MDR1 gene polymorphisms G2677T, and C3435T, but not C1236T were associated with the lipid lowering effect of atorvastatin among Jordanians.

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“…У носителей этого аллельного варианта (как гетерозигот, так и гомозигот) наблюдается сниже-ние экспрессии гена MDR1, что может приводить к сни-жению количества гликопротеина-Р в печени, кишеч-нике, почках и т.д. Данные некоторых исследований по-зволяют предположить, что полиморфизм гена MDR1 существенно не влияет на эффективность аторвастатина [9,10], хотя этот вопрос остается открытым.…”

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Effect of Genes Slco1b1 and Mdr1 Polymorphism on Atorvastatin Pharmacokinetics and Pharmacodynamics in Patients With Primary Hypercholesterolemia: Results of Pilot Pharmacogenetics Study

Семенов

Sichev

Кукес

2008

Racionalʹnaâ farmakoterapiâ v kardiologii

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Влияние полиморфизма генов SLCO1B1 и MDR1 на фармакокинетику и фармакодинамику аторвастатина у пациентов с первич-ной гиперхолестеринемией. Результаты пилотного фармакогенетического исследования А.В. Семенов, Д.А. Сычев, В.Г. Кукес Кафедра клинической фармакологии и пропедевтики внутренних болезней, Московская медицинская академия им. И.М. Сеченова Цель. Оценить влияние полиморфизма генов SLCO1B1 и MDR1 на фармакокинетику и фармакодинамику аторвастатина у пациентов с пер-вичной гиперхолестеринемией. Материал и методы. В исследовании принял участие 21 пациент (9 мужчин и 14 женщин; средний возраст 57 лет; все -европеоидной расы) с первичной гиперхолестеринемией (по критериям NCEP) с концентрацией общего холестерина крови более 5,9 ммоль/л после 4-недель-ной гиполипидемической диеты. Для оценки фармакокинетики в первый день лечения пациентам назначался аторвастатин в дозе 80 мг с забором проб крови до (0) и после приема препарата. Проведен скрининг на наличие полиморфизма генов MDR1 и SLCO1B1 с помощью полимеразной цепной реакции. Результаты. Выявлена меньшая эффективность лечения у носителей генотипа SLCO1B1 .с521СС по сравнению с другими генотипами, тог-да как полиморфизм гена MDR1 существенно не влиял на эффективность лечения. Не было выявлено связи между генотипом и частотой раз-вития нежелательных лекарственных реакций. Заключение. Носительство полиморфных аллелей генов, кодирующих белки-транспортеры лекарственных средств ( в первую очередь ОАТР-С) может существенно изменять фармакокинетические параметры (AUC) аторвастатина и индивидуальный ответ на лечение. Ключевые слова: полиморфизм генов белков-транспортеров, аторвастатин, фармакогенетика, гиперхолестеринемия. Aim. To study effects of genes SLCO1B1 and MDR1 polymorphism on atorvastatin pharmacokinetics and pharmacodynamics in patients with primary hypercholesterolemia. Material and methods. 21 patients (9 men and 14 women; 57 y.o. in average, all were Caucasians) with primary hypercholesterolemia (NCEP criteria) were involved in the study. All patients had total cholesterol plasma level >5.9 mmol/l after 4-week course of lipid-lowering diet. Atorvastatin (80 mg once daily in the first treatment day) was given to patients for pharmacokinetics estimation. Blood samples for analysis were taken before and after drug administration. Genes SLCO1B1 and MDR1 polymorphism screening was made by polymerase chain reaction. Results. Treatment efficacy in patients with SLCO1B1.с521СС genotype was less than this in patients with other genotypes. Genes MDR1 polymorphism have no influence on treatment efficacy. There is no correlation between genotype and drug adverse effects rate. Conclusion. Polymorphism of genes responsible for protein-transporters (first of all ОАТР-С) can significantly determine drug pharmacokinetic and individual response on atorvastatin therapy.

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High baseline serum total and LDL cholesterol levels are associated with MDR1 haplotypes in Brazilian hypercholesterolemic individuals of European descent

Cited by 55 publications

References 37 publications

Frequency of Common Variants in Genes Involved in Lipid-Lowering Response to Statins in Chilean Subjects with Hypercholesterolemia

Frequency of Common Variants in Genes Involved in Lipid-Lowering Response to Statins in Chilean Subjects with Hypercholesterolemia

The role of Multidrug Resistance-1 (MDR1) variants in response to atorvastatin among Jordanians

Effect of Genes Slco1b1 and Mdr1 Polymorphism on Atorvastatin Pharmacokinetics and Pharmacodynamics in Patients With Primary Hypercholesterolemia: Results of Pilot Pharmacogenetics Study

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