Breast cancer resistance protein (BCRP), also termed ABCG2, is a member of an ATP-binding cassette transporter
G family, which was originally identified in relation to drug resistance in cancer cells. BCRP intrinsically interacts
with a range of substances such as sterols, porphyrins and a variety of dietary compounds, but it mediates extrusion of
toxic compounds out of cells and underlies multidrug resistance of cancer cells. Hence, BCRP expression levels in tumor
and non-tumor cells may determine response to chemotherapy as well as adverse effects. In the former part of this paper,
the latest findings are reviewed regarding clinical significance of BCRP expression in malignancy. In the latter part, reports
on single nucleotide polymorphisms (SNPs) of the BCRP gene are reviewed focusing on impacts upon cancer chemotherapy.
C421A and C376T, which result in very low and null expression of the protein, respectively, are particularly
referred to regarding their phenotypes because of possible importance in cancer chemotherapy. Approximately one tenth
of hyperuricemia/gout patients and a considerable part of population with Junior a (-) [jr(a-)] blood type are expected to
bear these SNPs on the both alleles. Therefore, genotypic examination of the BCRP gene would be recommended in these
populations before the start of chemotherapy including BCRP substrate drugs.
Keywords: ABCG2, anticancer drug, BCRP, C376T, C421A, cancer, chemotherapy, clinical significance, drug resistance,
gout, jr(a-), malignancy, SNPs.
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