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Detection of single nucleotide polymorphisms in the ABCG2 gene in a Dutch population.

Tessa M Bosch ,
Linda M Kjellberg ,
Anja Bouwers ,
Bobby P C Koeleman ,
Jan H M Schellens ,
Jos H Beijnen ,
Paul H M Smits ,
Irma Meijerman

Abstract

METHODS

Blood samples were obtained from 100 healthy volunteers to isolate genomic DNA. PCR amplification was performed, followed by DNA sequencing. The population, of which the ethnicity was 93% Caucasian, consisted of 79 female individuals and 21 males.

CONCLUSIONS

The results will be used in future studies to explore the influence of the different SNPs on ABCG2 protein expression, activity, and substrate specificity. In addition, the results can be used to study the effects of genetic polymorphisms in the ABCG2 gene on the pharmacokinetic profile of anticancer drugs.

RESULTS

In total, 19 SNPs were found in the ABCG2 gene, of which 7 were previously unknown. The SNPs G8883A in exon 5 and C44168T in exon 14 cause an amino acid change of R160Q and R575X, respectively. Most of the previously unknown SNPs were found in introns.

BACKGROUND

ABCG2 is a drug transporter involved in the protection of tissues by actively transporting toxic substances and xenobiotics out of cells. Cancer cells overexpressing the ABCG2 gene show multidrug resistance to mitoxantrone-, methotrexate-, doxorubicin-, and camptothecin-based anticancer drugs, such as topotecan and SN-38. Large interindividual differences have been shown in oral availability and clearance of drugs that are substrates for ABCG2. Variation in the ABCG2 gene, such as single nucleotide polymorphisms (SNPs), can possibly explain the variability in pharmacokinetics of ABCG2 substrates.

AIM

This study was performed to screen for SNPs in the ABCG2 gene to determine the frequencies of currently known and previously unknown SNPs in a Dutch population.

More about this publication

American journal of pharmacogenomics : genomics-related research in drug development and clinical practice

Volume 5
Issue nr. 2
Pages 123-31
Publication date 09-04-2005

Full text links

Publisher website (DOI) 10.2165/00129785-200505020-00005
Europe PubMed Central 15813675
Pubmed 15813675

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