Aug 22, 2002 the pharmacokinetics of digoxin was studied in 15 healthy volunteers, who were divided into 3 groups n 5 each on the basis of genotyping for the mdr1 gene, in a 4. Abcb1 and slco1b3 gene polymorphisms and their impact on. Suggestive evidence for linkage at chromosome 7q has been reported for both cd and uc. Mdr1 gene expression is also modulated by p53 scotto 2003. Absence of association between mdr1 genetic polymorphisms. Structure, function, expression, genomic organization, and. Mdr1 genotyperelated pharmacokinetics and pharmacodynamics. Ivermectin sensitivity in collies is associated with a deletion mutation of the mdr1 gene. The importance of mdr1 gene polymorphisms for tacrolimus. Frontiers effects of genetic polymorphisms of drug. Mar 01, 2003 digoxin pharmacokinetics and mdr1 genetic polymorphisms digoxin pharmacokinetics and mdr1 genetic polymorphisms verstuyft, celine. More formally, it is an atpdependent efflux pump with broad substrate. Association of the multidrug resistance1 gene single jasn. Significant genetic linkage of mdr1 polymorphisms at positions 3435 and 2677.
Effects of genetic polymorphisms on the pharmacokinetics of. To clarify the relationships between mdr1 genetic polymorphisms in exon 26 c3435t and 21 g2677ta and digoxin pharmacokinetics. The effect of mdr1 c3435t single nucleotide polymorphism snp in exon 26 on digoxin pharmacokinetics has recently been challenged. Association of mdr1 gene polymorphisms with pharmacokinetics of tacrolimus. The pharmacokinetics of indinavir were best described by a onecompartment model with firstorder absorption. Digoxin pharmacokinetics and mdr1 genetic polymorphisms digoxin pharmacokinetics and mdr1 genetic polymorphisms verstuyft, celine.
It was reported that the cc genotype 6 months posttransplant. Mdr1 gene encodes for p glycoprotein pgp, which plays an important role. Mdr1 has a crucial role in drug disposition, and genetic polymorphisms in this gene might alter the pharmacokinetics and bioavailability of a diverse range of pgp substrates kurose et al. Significant genetic linkage of mdr1 polymorphisms at. A prospective analysis author links open overlay panel inwha kim phd 1 hwiyeol yun phd 2 boyoon choi ms 1 nayoung han ms 1 seonyang park md, phd 3 eun sook lee pharmd 4 jung mi oh pharmd 1.
Pharmacogenetics of drug transporters and its impact on the. Plasma levels of atazanavir and the risk of hyperbilirubinemia are. Impact of abcb1 mdr1 gene polymorphism and pglycoprotein. Abcb1 gene polymorphism on digoxin pharmacokinetics is still not clear, as the results of different studies mainly in healthy individuals are contradictory 1, 4, 6, 8, 11, 15, 20, 21. Recent clinical studies suggest the importance of the mdr1 genotype at position 3435 c3435t in terms of pharmacokinetics, but there is still no consensus in reports on the relationship between the genotype and plasmaserum concentrationtime profiles of drugs after conventional oral administration. Dec 01, 2006 a cytosinetoguanine polymorphism found at location 3435 in exon 26 c3435t of the mdr1 abcb1 gene is found in 1617% of individuals from african descent, in 5060% of caucasians, and in 4070% of asians. Crohn disease cd and ulcerative colitis uc are overlapping chronic inflammatory bowel diseases ibds. For the mdr1 c3435t polymorphism, cc, ct, and tt genotypes were detected in 15 50. Abcb1 gene variants, digoxin and risk of sudden cardiac. Polymorphisms of mdr1 gene have been reported to be associated with the expression level of pgp. A literature search was conducted in july 2007 to locate the relevant papers by using the pubmed electronic source from 1997 and onwards. With the sequencing of the human genome, it has been estimated that approximately 5001200 genes code for drug transporters. The objective of the present study was to determine whether mdr1 genetic polymorphisms in exons 21 and 26 g2677ta and c3435t are in association with indinavir idv plasma concentrations. Influence of abcb1 gene polymorphisms on the pharmacokinetics.
However, a recent study showing an association between haplotypes of the mdr1 gene and the steadystate kinetics of the pgp substrate digoxin showed that mdr1 polymorphisms were significantly associated with the absorption but not with the elimination of the drug, suggesting that the snp action occurred mainly in the gut 24. Metaanalysis of the influence of mdr1 c3435t polymorphism on. The aim of this study was to examine the relationship between mdr1 gene single nucleotide polymorphisms snps and their haplotypes with dosage of tacrolimus in kidney transplant recipients who were cytochrome cyp 3a53 homozygotes. Pglycoprotein polymorphism and levothyroxine bioavailability. Request pdf digoxin pharmacokinetics and mdr1 genetic polymorphisms the effect of mdr1 c3435t single nucleotide polymorphism. Pglycoprotein function due to polymorphisms of mdr1. To evaluate the mdr1 genotype frequency in the japanese population and to study the relationship between the mdr1 genotype and the pharmacokinetics of digoxin after single oral administration in healthy subjects. View the article pdf and any associated supplements and figures for a period of 48 hours. The relationship between mdr1 single nucleotide polymorphisms snp and the pharmacokinetic or pharmacodynamic responses to protease inhibitors has been recently challenged aim. Feb 15, 2016 polymorphisms of the multi drug resistance mdr1 gene cause variability in pglycoprotein mediated metabolism of tacrolimus. Aims studies revealing conflicting results of the functional significance of mdr1 exon 26 c3435t snp on the disposition of digoxin in different ethnic groups led us to perform a meta. Mdr1 genotypes for c3435t and g2677ta snps were determined in 32 healthy subjects whose single oral dose digoxin pharmacokinetics had been measured over 48 h. In the final model, the mdr1 c3435t genotype and ritonavir were identified as statistically significant covariates p.
Recently, functional genetic polymorphisms in the mdr1 gene have been identified. Our results confirm that the mdr1 c3435t single nucleotide polymorphism snp significantly affects digoxin disposition kinetics, with homozygous tt subjects. Efflux transporters like mdr1 and mrp2 may modulate the pharmacokinetics of about 50 % of all drugs. Mdr1 genotyperelated duodenal absorption rate of digoxin in. Therefore, we recruited subjects with simultaneous wild, heterozygous, or mutant types of the mdr1 gene at positions 2677. Genetic polymorphisms can cause pharmacokinetic variability which may also be responsible for the observed suboptimal response. Effect of cyp2d6, cyp3a5, and mdr1 genetic polymorphisms on the pharmacokinetics of risperidone and its active moiety. Abcb1 ethnicity and genetic polymorphisms in the mdr1, genotype of the donor but not of the recipient is a major cyp3a4, and cyp3a5 genes. To investigate the relationship between c3435t snp and cyclosporine pharmacokinetics, the following keywords were used. Xiv, issue 1 the c and t alleles of the mdr1 multiple drug resistance 1 c3435t polymorphism share similar frequencies in the romanian population a. An integrated pharmacokineticpharmacogenomic analysis of. Digoxin pharmacokinetics and mdr1 genetic polymorphisms.
The study was carried out in 77 patients diagnosed with congestive heart failure administered di. In experiments with mdr1 ko mice, substrates of mdr1 e. Genetic polymorphisms in both genes may explain interindividual. The genotypes of polymorphic position c3435t were determined by pcrrflp. Genotyping was carried out on 116 unrelated jordanian and 1 sudanese subjects. The aim of the present study was to evaluate the effects of abcb1 gene polymorphism on steadystate digoxin serum concentration in congestive heart fail. Tacrolimus dose requirement in relation to donor and. Pdf association of the multidrug resistance1 gene single. Sep 01, 2009 significant genetic linkage of mdr1 polymorphisms at positions 3435 and 2677. Suppression of mdr1 expression by normal p53 is suggested to be through direct interaction of p53 protein with a novel ciselement in the proximal promoter of mdr1 gene 4072. Gp, between carriers and noncarriers of haplotypes between g2677t and c3435t. Describe classes of drugs whose pharmacokinetics are affected by indi vidual transporters.
Effect of grapefruit juice on digoxin pharmacokinetics in humans. Numerous genetic polymorphisms in mdr1 have been described, some of which have been. Mdr1 genotypes do not influence the absorption of a single oral. Genetic polymorphisms in mdr1, cyp3a4 and cyp3a5 genes. Mdr1 gene encodes for the atpdependent membrane efflux transport for pglycoprotein, and it was shown that mdr1 polymorphisms could affect the pharmacokinetics of digoxin 30, 31. Minimal effect of mdr1 and cyp3a5 genetic polymorphisms on. Pdf digoxin, a drug of narrow therapeutic index, is a substrate for common. Effect of cyp2d6, cyp3a5, and mdr1 genetic polymorphisms. Analysis of the effect of mdr1 c3435t polymorphism on. Popp1, mariela sanda militaru1, tania octavia crisan1, m. Aims the c3435t polymorphism in the human mdr1 gene is associated with lower intestinal p. The hematological side effects of paclitaxel were intensified by gemcitabine, and were correlated with paclitaxel pharmacokinetics. Since several other polymorphisms have been found in the mdr1 gene 14, 21, 22 subjects.
Pdf multidrug resistance gene1 mdr1 haplotypes and the. Metaanalysis of the influence of mdr1 c3435t polymorphism. Aug 01, 2012 abcb1 c3435t genetic polymorphism on population pharmacokinetics of methotrexate after hematopoietic stem cell transplantation in korean patients. Pglycoprotein pgp is a membrane protein that functions as an adenosine triphosphatedependent efflux pump for xenobiotics at the bloodbrain barrier bbb. We therefore compared fexofenadine kinetics between subjects with the tt genotype of the human mdr1 gene at position 3435 and individuals homozygous for the wildtype allele. Pop1, anca dana buzoianu2 1 department of medical genetics.
Several drugs, substrates of mdr1, display altered pharmacokinetics if coadministered with mdr1 inhibitors or in mice that do not express this protein schinkel et al. Studies on pharmacokinetic mechanism of phenytoin resistance in. Metaanalysis of the influence of mdr1 c3435t polymorphism on digoxin pharmacokinetics and mdr1 gene expression. It has been suggested that abcb1 polymorphism, as well as coadministration of pglyco protein inhibitors, may influence digoxin bioavailability. Aug 20, 2007 neither the polymorphisms at exon 26 c3435t and at exon 21 g2677at in mdr1 nor the cyp3a51 allele significantly affected the total body clearance of paclitaxel. Mdr1 genotyperelated pharmacokinetics of digoxin after. Functional significance of genetic polymorphisms in pglycoprotein mdr1, abcb1 and breast cancer resistance protein bcrp, abcg2 drug metab pharmacokinet. Mdr1 gene encodes for p glycoprotein pgp, which plays an important role in bioavailability and celltoxicity limitation of a wide range of drugs and xenobiotics. Feb 01, 2018 pgp is encoded by the mdr1 gene, which is located in the region 7q21. Impact of genetic variation in breast cancer resistance. Low heritability in pharmacokinetics of talinolol core. Pdf multidrug resistance gene1 mdr1 haplotypes and. Three single nucleotide polymorphisms snps in the coding region c3435t, c1236t and g2677ta are the most widely studied snps in mdr1 and have been related to substrate.
The genetic polymorphisms of htr2c 759ct, abcb1 1236ct, abcb1 2677gta, and abcb1 3435ct were not associated with overweightobesity in children and. This study was performed to elucidate the effects of c3435t on the rate of duodenal. Evaluation of in vivo pglycoprotein function at the blood. Mdr1 gene polymorphisms and clinical relevance sciencedirect. The objectives were detection of the mdr1 gene c3435t polymorphism at exon 26, the frequency of each genotype, and its relation to digoxin blood level in cardiac patients under digoxin therapy. The effect of mdr1 polymorphism on digoxin absorption has been probe. The 3435crt polymorphism at the multidrug resistance gene 1 mdr1 was examined in 74 patients with human. Digoxin and mexiletine sensitivity in a collie with the mdr1. Concepts in pharmacogenomics sample chapter 5 ashp. Genetic polymorphisms in mdr1, cyp3a4 and cyp3a5 genes in a.
Feb 05, 2008 digoxin and mexiletine sensitivity in a collie with the mdr1 mutation. Mdr1 gene polymorphism has also been suggested to affect the therapy. Pdf polymorphisms of the abcb1 gene are associated with the. The mdr1 genotype at exon 26 was determined in 114 healthy volunteers by polymerase chain reactionrestriction fragment length polymorphism. To investigate the relationship between c3435t snp and digoxin pharmacokinetics, the following keywords were used. Multiple drug resistant1 gene c3435t polymorphism and its. Whereas wildtype p53 suppresses mdr1 expression, many p53 mutants are able to activate mdr1 expression. Contained within this region is the gene for mdr1 multidrug resistance, a membrane transport protein for which human polymorphisms have been reported in ala893serthr and c3435t that alter. Pgp is the product of multidrug resistance gene mdr1 abcb1.
Role of snp and digoxin response in atrial fibrillation. Mar, 2007 read modelling the influence of mdr1 polymorphism on digoxin pharmacokinetic parameters, european journal of clinical pharmacology on deepdyve, the largest online rental service for scholarly research with thousands of academic publications available at your fingertips. Pglycoprotein 1 permeability glycoprotein, abbreviated as pgp or pgp also known as multidrug resistance protein 1 mdr1 or atpbinding cassette subfamily b member 1 abcb1 or cluster of differentiation 243 cd243 is an important protein of the cell membrane that pumps many foreign substances out of cells. Cyp3a5 producers and genotype pgp is a drug transporter which is the product cyp3a533 nonproducers. These results suggest that the digoxin rifampicin interaction mainly occurs at the intestinal level and that. The aim of the present study was to evaluate the effects of abcb1 mdr1 gene polymorphism on pglycoprotein model substrate, i. In this study we assessed the heritability of the pharmacokinetics of talinolol as a putative probe drug for mdr1. Functional significance of genetic polymorphisms in p. It is a silent mutation, but is associated with altered pglycoprotein expression, and subsequently its substrate drug pharmacokinetics. Digoxin and mexiletine sensitivity in a collie with the. Request pdf on nov 1, 2002, masanori horinouchi and others published significant genetic linkage of mdr1 polymorphisms at positions 3435 and 2677.
Functional relevance to pharmacokinetics of digoxin. The aim of this study was to determine the genotype and allele frequencies of mdr1 gene c3435t polymorphism in jordanian and sudanese populations, and to compare them with the frequencies established in various ethnic groups. Modelling the influence of mdr1 polymorphism on digoxin. Role of human mdr1 gene polymorphism in bioavailability and.
Concerning the effects of genetic polymorphisms on pharmacotherapy, the best characterized drug transporter is the multidrug resistant transporter pglycoproteinmdr1, the gene product of mdr1. With regard to the variability, polymorphisms of the mdr1 gene have. Jul 21, 2006 the authors demonstrated that there are significant differences in the pharmacokinetics of digoxin, a substrate of p. Functional implications of genetic polymorphisms in the multidrug. Mdr1 ala893 polymorphism is associated with inflammatory. The host and the parasite do have mdr1 and cyp3a genes and some workers have postulated that parasite mdr1 gene may be contributing towards drug inefficacy 28.
Functional relevance to pharmacokinetics of digoxin masanori horinouchi 1 toshiyuki sakaeda 1. Mdr1 genetic polymorphisms and tacrolimus pharmacokinetics. Influence of cyp3a5 and mdr1 abcb1 polymorphisms on the ph. Relate genetic variants of transport proteins to variations in drug ac. Abcb1 polymorphism, pglycoprotein, digoxin, genetic polymorphism, inhibitors. With regard to the variability, polymorphisms of the mdr1 gene have recently been reported to be associated with alterations in disposition kinetics and interaction profiles of clinically useful drugs, including digoxin, fexofenadine, ciclosporin and talinolol. Combinations of common snps of the transporter gene abcb1. Department of pharmacy, peking university first hospital, beijing, china.
Aims a noncoding single nucleotide polymorphism snp in exon 26 3435c t. The pharmacokinetics of digoxin was studied in 15 healthy volunteers, who were divided into 3 groups n 5 each on the basis of genotyping for the mdr1 gene, in a 4dose study after single doses of digoxin alone 0. Mdr1 genotypes for c3435t and g2677ta snps were determined in 32 healthy subjects whose single oral dose digoxin pharmacokinetics. Amlodipine, but not mdr1 polymorphisms, alters the.
Effects of different genotypes on the pharmacokinetics of probe substrates may. It is currently unknown how much of the variation in the activities of important drug membrane transporters like mdr1 or mrp2 is determined by genetic or by environmental factors. Minimal effect of mdr1 and cyp3a5 genetic polymorphisms on the pharmacokinetics. Role of human mdr1 gene polymorphism in bioavailability. Effect of abcb1 mdr1 haplotypes derived from g2677tc3435t. Polymorphisms in the abc drug transporter gene mdr1 nature.
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