Literature DB >> 18300232

6-mercaptopurine and 9-(2-phosphonyl-methoxyethyl) adenine (PMEA) transport altered by two missense mutations in the drug transporter gene ABCC4.

Daniel Janke1, Sherif Mehralivand, Dennis Strand, Ute Gödtel-Armbrust, Alice Habermeier, Ulrike Gradhand, Christine Fischer, Mohammad R Toliat, Peter Fritz, Ulrich M Zanger, Matthias Schwab, Martin F Fromm, Peter Nürnberg, Leszek Wojnowski, Ellen I Closs, Thomas Lang.   

Abstract

Multiple drug resistance protein 4 (MRP4, ABCC4) belongs to the C subfamily of the ATP-binding cassette (ABC) transporter superfamily and participates in the transport of diverse antiviral and chemotherapeutic agents such as 6-mercaptopurine (6-MP) and 9-(2-phosphonyl methoxyethyl) adenine (PMEA). We have undertaken a comprehensive functional characterization of protein variants of MRP4 found in Caucasians and other ethnicities. A total of 11 MRP4 missense genetic variants (nonsynonymous SNPs), fused to green fluorescent protein (GFP), were examined in Xenopus laevis oocytes for their effect on expression, localization, and function of the transporter. Radiolabeled 6-MP and PMEA were chosen as transport substrates. All MRP4 protein variants were found to be expressed predominantly in the oocyte membrane. A total of four variants (Y556C, E757 K, V776I, and T1142 M) exhibited a 20% to 40% reduced expression level compared to the wild type. Efflux studies showed that 6-MP is transported by MRP4 in unmodified form. Compared to wild-type MRP4, the transmembrane variant V776I, revealed a significant lower activity in 6-MP transport, while the amino acid exchange Y556C in the Walker(B) motif displayed significantly higher transport of PMEA. The transport properties of the other variants were comparable to wild-type MRP4. Our study shows that Xenopus oocytes are well suited to characterize MRP4 and its protein variants. Carriers of the rare MRP4 variants Y556C and V776I may have altered disposition of MRP4 substrates.

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Year:  2008        PMID: 18300232     DOI: 10.1002/humu.20694

Source DB:  PubMed          Journal:  Hum Mutat        ISSN: 1059-7794            Impact factor:   4.878


  17 in total

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4.  Deregulated hepatic metabolism exacerbates impaired testosterone production in Mrp4-deficient mice.

Authors:  Jessica A Morgan; Satish B Cheepala; Yao Wang; Geoff Neale; Masashi Adachi; Deepa Nachagari; Mark Leggas; Wenchen Zhao; Kelli Boyd; Raman Venkataramanan; John D Schuetz
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5.  Multidrug resistance protein 4 (MRP4) polymorphisms impact the 6-mercaptopurine dose tolerance during maintenance therapy in Japanese childhood acute lymphoblastic leukemia.

Authors:  Y Tanaka; A Manabe; H Fukushima; R Suzuki; H Nakadate; K Kondoh; K Nakamura; K Koh; T Fukushima; M Tsuchida; K Koike; N Kiyokawa; E Noguchi; R Sumazaki; T Komiyama
Journal:  Pharmacogenomics J       Date:  2014-11-18       Impact factor: 3.550

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Authors:  Ji Eun Park; Gongmi Ryoo; Wooin Lee
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7.  Crucial role for phylogenetically conserved cytoplasmic loop 3 in ABCC4 protein expression.

Authors:  Satish B Cheepala; Ju Bao; Deepa Nachagari; Daxi Sun; Yao Wang; Tao P Zhong; Tao Zhong; Anjaparavanda P Naren; Jie Zheng; John D Schuetz
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8.  Thiopurine pharmacogenomics: association of SNPs with clinical response and functional validation of candidate genes.

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Journal:  Pharmacogenomics       Date:  2014-03       Impact factor: 2.533

9.  ABCC4/MRP4: a MYCN-regulated transporter and potential therapeutic target in neuroblastoma.

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10.  Quantitative Evaluation of Drug Resistance Profile of Cells Expressing Wild-Type or Genetic Polymorphic Variants of the Human ABC Transporter ABCC4.

Authors:  Megumi Tsukamoto; Shiori Sato; Kazuhiro Satake; Mizuki Miyake; Hiroshi Nakagawa
Journal:  Int J Mol Sci       Date:  2017-07-04       Impact factor: 5.923

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