Your search keyword '"Wijnholds J"' showing total 12 results

1. Mice lacking Mrp3 (Abcc3) have normal bile salt transport, but altered hepatic transport of endogenous glucuronides.

Author

Zelcer N, van de Wetering K, de Waart R, Scheffer GL, Marschall HU, Wielinga PR, Kuil A, Kunne C, Smith A, van der Valk M, Wijnholds J, Elferink RO, and Borst P

Subjects

Animals, Bile Ducts physiopathology, Bilirubin analogs & derivatives, Bilirubin blood, Biological Transport genetics, Biological Transport physiology, Cholic Acids metabolism, Deoxycholic Acid metabolism, Ileum metabolism, Immunoblotting, Immunohistochemistry, Ligation, Liver chemistry, Male, Mice, Mice, Inbred Strains, Multidrug Resistance-Associated Proteins analysis, Multidrug Resistance-Associated Proteins genetics, Taurocholic Acid metabolism, Bile Acids and Salts metabolism, Glucuronides metabolism, Liver metabolism, Multidrug Resistance-Associated Proteins deficiency, Multidrug Resistance-Associated Proteins physiology

Abstract

Background/aim: Multidrug Resistance Protein 3 (MRP3) transports bile salts and glucuronide conjugates in vitro and is postulated to protect the liver in cholestasis. Whether the absence of Mrp3 affects these processes in vivo is tested., Methods: Mrp3-deficient mice were generated and the contribution of Mrp3 to bile salt and glucuronide conjugate transport was tested in (1): an Ussing-chamber set-up with ileal explants (2), the liver during bile-duct ligation (3), liver perfusion experiments, and (4) in vitro vesicular uptake experiments., Results: The Mrp3((-/-)) mice show no overt phenotype. No differences between WT and Mrp3-deficient mice were found in the trans-ileal transport of taurocholate. After bile-duct ligation, there were no differences in histological liver damage and serum bile salt levels between Mrp3((-/-)) and WT mice, but Mrp3-deficient mice had lower serum bilirubin glucuronide concentrations. Glucuronide conjugates of hyocholate and hyodeoxycholate are substrates of MRP3 in vitro and in livers that lack Mrp3, there is reduced sinusoidal secretion of hyodeoxycholate-glucuronide after perfusion with hyodeoxycholate., Conclusions: Mrp3 does not have a major role in bile salt physiology, but is involved in the transport of glucuronidated compounds, which could include glucuronidated bile salts in humans.

Published

2006

2. The multidrug resistance protein 1 (Mrp1), but not Mrp5, mediates export of glutathione and glutathione disulfide from brain astrocytes.

Author

Minich T, Riemer J, Schulz JB, Wielinga P, Wijnholds J, and Dringen R

Subjects

Animals, Animals, Newborn, Astrocytes drug effects, Blotting, Northern methods, Cell Survival genetics, Dose-Response Relationship, Drug, Enzyme Inhibitors pharmacology, Hydrogen Peroxide pharmacology, Leukotriene Antagonists pharmacology, Mice, Mice, Knockout, Minor Histocompatibility Antigens pharmacology, Multidrug Resistance-Associated Proteins deficiency, Propionates pharmacology, Protein Transport, Quinolines pharmacology, RNA, Messenger metabolism, Reverse Transcriptase Polymerase Chain Reaction methods, Time Factors, Astrocytes metabolism, Brain cytology, Glutathione metabolism, Glutathione Disulfide metabolism, Multidrug Resistance-Associated Proteins metabolism

Abstract

Astrocytes play an important role in the glutathione (GSH) metabolism of the brain. To test for an involvement of multidrug resistance protein (Mrp) 1 and 5 in the release of GSH and glutathione disulfide (GSSG) from astrocytes, we used astrocyte cultures from wild-type, Mrp1-deficient [Mrp1(-/-)] and Mrp5-deficient [Mrp5(-/-)] mice. During incubation of wild-type or Mrp5(-/-) astrocytes, GSH accumulated in the medium at a rate of about 3 nmol/(h.mg), whereas the export of GSH from Mrp1(-/-) astrocytes was only one-third of that. In addition, Mrp1(-/-) astrocytes had a 50% higher specific GSH content than wild-type or Mrp5(-/-) cells. The presence of 50 microm of the Mrp inhibitor MK571 inhibited the rate of GSH release from wild-type and Mrp5(-/-) astrocytes by 60%, but stimulated at the low concentration of 1 microm GSH release by 40%. In contrast, both concentrations of MK571 did not affect GSH export from Mrp1(-/-) astrocytes. Moreover, in contrast to wild-type and Mrp5(-/-) cells, GSSG export during H(2)O(2) stress was not observed for Mrp1(-/-) astrocytes. These data demonstrate that in astrocytes Mrp1 mediates 60% of the GSH export, that Mrp1 is exclusively responsible for GSSG export and that Mrp5 does not contribute to these transport processes.

Published

2006

3. The human multidrug resistance protein MRP5 transports folates and can mediate cellular resistance against antifolates.

Author

Wielinga P, Hooijberg JH, Gunnarsdottir S, Kathmann I, Reid G, Zelcer N, van der Born K, de Haas M, van der Heijden I, Kaspers G, Wijnholds J, Jansen G, Peters G, and Borst P

Subjects

Biological Transport, Cell Line, Humans, Polyglutamic Acid pharmacokinetics, Substrate Specificity, Folic Acid pharmacokinetics, Folic Acid Antagonists pharmacokinetics, Methotrexate analogs & derivatives, Methotrexate pharmacokinetics, Multidrug Resistance-Associated Proteins metabolism, Polyglutamic Acid analogs & derivatives

Abstract

Members of the multidrug resistance protein family, notably MRP1-4/ABCC1-4, and the breast cancer resistance protein BCRP/ABCG2 have been recognized as cellular exporters for the folate antagonist methotrexate (MTX). Here we show that MRP5/ABCC5 is also an antifolate and folate exporter based on the following evidence: (a) Using membrane vesicles from HEK293 cells, we show that MRP5 transports both MTX (KM = 1.3 mmol/L and VMAX = 780 pmol per mg protein per minute) and folic acid (KM = 1.0 mmol/L and VMAX = 875 pmol per mg protein per minute). MRP5 also transports MTX-glu2 (KM = 0.7 mmol/L and VMAX = 450 pmol per mg protein per minute) but not MTX-glu3. (b) Both accumulation of total [3H]MTX and of MTX polyglutamates were significantly reduced in MRP5 overexpressing cells. (c) Cell growth inhibition studies with MRP5 transfected HEK293 cells showed that MRP5 conferred high-level resistance (>160-fold) against the antifolates MTX, GW1843, and ZD1694 (raltitrexed) in short-term (4 hours) incubations with high drug concentrations; this resistance was proportional to the MRP5 level. (d) MRP5-mediated resistance (8.5- and 2.1-fold) was also found in standard long-term incubations (72 hours) at low concentrations of ZD1694 and GW1843. These results show the potential of MRP5 to mediate transport of (anti)folates and contribute to resistance against antifolate drugs.

Published

2005

4. The potential impact of drug transporters on nucleoside-analog-based antiviral chemotherapy.

Author

Borst P, Balzarini J, Ono N, Reid G, de Vries H, Wielinga P, Wijnholds J, and Zelcer N

Subjects

Biological Transport, Active physiology, Nucleotides, Cyclic metabolism, Nucleotides, Cyclic pharmacology, Antiviral Agents metabolism, Antiviral Agents pharmacology, Drug Resistance, Viral, Multidrug Resistance-Associated Proteins physiology, Nucleosides metabolism, Nucleosides pharmacology

Abstract

Several ATP-binding cassette (ABC) transporters can transport drugs out of cells against steep concentration gradients resulting in resistance to the drugs transported. Recent work has shown that at least three members of the family of human Multidrug Resistance-associated Proteins (MRPs), MRP4, 5 and 8, are able to transport some nucleoside-monophosphate analogs. This can result in resistance to the base, nucleoside or nucleotide precursors of these results, at least in cell lines with high levels of transporter. The affinity of these transporters for the nucleotide analogs studied thus far is relatively low (millimolar rather than micromolar), and this limits their potential impact on the resistance. We briefly review how ABC transporters in general, and MRPs in particular, could affect the disposition and cellular accumulation of antiviral compounds.

Published

2004

5. The human multidrug resistance protein MRP4 functions as a prostaglandin efflux transporter and is inhibited by nonsteroidal antiinflammatory drugs.

Author

Reid G, Wielinga P, Zelcer N, van der Heijden I, Kuil A, de Haas M, Wijnholds J, and Borst P

Subjects

Adenosine Triphosphate metabolism, Alprostadil metabolism, Animals, Biological Transport, Cell Line, Cell Membrane metabolism, Diffusion, Dinoprost metabolism, Dinoprostone metabolism, Dose-Response Relationship, Drug, Humans, Insecta, Prostaglandins A metabolism, Prostaglandins F metabolism, RNA Interference, RNA, Small Interfering metabolism, Thromboxane B2 metabolism, Time Factors, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Multidrug Resistance-Associated Proteins, Prostaglandins metabolism, Ribosomal Proteins chemistry, Ribosomal Proteins physiology

Abstract

Prostaglandins are involved in a wide variety of physiological and pathophysiological processes, but the mechanism of prostaglandin release from cells is not completely understood. Although poorly membrane permeable, prostaglandins are believed to exit cells by passive diffusion. We have investigated the interaction between prostaglandins and members of the ATP-binding cassette (ABC) transporter ABCC [multidrug resistance protein (MRP)] family of membrane export pumps. In inside-out membrane vesicles derived from insect cells or HEK293 cells, MRP4 catalyzed the time- and ATP-dependent uptake of prostaglandin E1 (PGE1) and PGE2. In contrast, MRP1, MRP2, MRP3, and MRP5 did not transport PGE1 or PGE2. The MRP4-mediated transport of PGE1 and PGE2 displayed saturation kinetics, with Km values of 2.1 and 3.4 microM, respectively. Further studies showed that PGF1alpha, PGF2alpha, PGA1, and thromboxane B2 were high-affinity inhibitors (and therefore presumably substrates) of MRP4. Furthermore, several nonsteroidal antiinflammatory drugs were potent inhibitors of MRP4 at concentrations that did not inhibit MRP1. In cells expressing the prostaglandin transporter PGT, the steady-state accumulation of PGE1 and PGE2 was reduced proportional to MRP4 expression. Inhibition of MRP4 by an MRP4-specific RNA interference construct or by indomethacin reversed this accumulation deficit. Together, these data suggest that MRP4 can release prostaglandins from cells, and that, in addition to inhibiting prostaglandin synthesis, some nonsteroidal antiinflammatory drugs might also act by inhibiting this release.

Published

2003

6. Pseudoxanthoma elasticum: a clinical, histopathological, and molecular update.

Author

Hu X, Plomp AS, van Soest S, Wijnholds J, de Jong PT, and Bergen AA

Subjects

Animals, Humans, Molecular Biology, Retinal Diseases genetics, Retinal Diseases pathology, Multidrug Resistance-Associated Proteins genetics, Mutation, Pseudoxanthoma Elasticum genetics, Pseudoxanthoma Elasticum pathology

Abstract

Pseudoxanthoma elasticum is an autosomally inherited disorder that is associated with the accumulation of mineralized and fragmented elastic fibers in the skin, Bruch's membrane in the retina, and vessel walls. The ophthalmic and dermatologic expression of pseudoxanthoma elasticum and its vascular complications are heterogeneous, with considerable variation in phenotype, progression, and mode of inheritance. Using linkage analysis and mutation detection techniques, mutations in the ABCC6 gene were recently implicated in the etiology of pseudoxanthoma elasticum. ABCC6 encodes the sixth member of the ATP-binding cassette transporter and multidrug resistance protein family (MRP6). In humans, this transmembrane protein is highly expressed in the liver and kidney. Lower expression was found in tissues affected by pseudoxanthoma elasticum, including skin, retina, and vessel walls. So far, the substrates transported by the ABCC6 protein and its physiological role in the etiology of pseudoxanthoma elasticum are not known. A functional transport study of rat MRP6 suggests that small peptides such as the endothelin receptor antagonist BQ123 are transported by MRP6. Similar molecules transported by ABCC6 in humans may be essential for extracellular matrix deposition or turnover of connective tissue at specific sites in the body. One of these sites is Bruch's membrane. This review is an update on etiology of pseudoxanthoma elasticum, including its clinical and genetic features, pathogenesis, and biomolecular basis.

Published

2003

7. Characterization of the MRP4- and MRP5-mediated transport of cyclic nucleotides from intact cells.

Author

Wielinga PR, van der Heijden I, Reid G, Beijnen JH, Wijnholds J, and Borst P

Subjects

1-Methyl-3-isobutylxanthine pharmacology, Blotting, Western, Cell Line, Cyclic AMP metabolism, Cyclic GMP metabolism, Dose-Response Relationship, Drug, Glutathione metabolism, Humans, Multidrug Resistance-Associated Proteins chemistry, Nitric Oxide metabolism, Nitric Oxide Donors pharmacology, Nitroprusside pharmacology, Phosphodiesterase Inhibitors pharmacology, Ribosomal Proteins chemistry, Time Factors, Biological Transport, Multidrug Resistance-Associated Proteins metabolism, Ribosomal Proteins metabolism

Abstract

Cyclic nucleotides are known to be effluxed from cultured cells or isolated tissues. Two recently described members of the multidrug resistance protein family, MRP4 and MRP5, might be involved in this process, because they transport the 3',5'-cyclic nucleotides, cAMP and cGMP, into inside-out membrane vesicles. We have investigated cGMP and cAMP efflux from intact HEK293 cells overexpressing MRP4 or MRP5. The intracellular production of cGMP and cAMP was stimulated with the nitric oxide releasing compound sodium nitroprusside and the adenylate cyclase stimulator forskolin, respectively. MRP4- and MRP5-overexpressing cells effluxed more cGMP and cAMP than parental cells in an ATP-dependent manner. In contrast to a previous report we found no glutathione requirement for cyclic nucleotide transport. Transport increased proportionally with intracellular cyclic nucleotide concentrations over a calculated range of 20-600 microm, indicating low affinity transport. In addition to several classic inhibitors of organic anion transport, prostaglandins A(1) and E(1), the steroid progesterone and the anti-cancer drug estramustine all inhibited cyclic nucleotide efflux. The efflux mediated by MRP4 and MRP5 did not lead to a proportional decrease in the intracellular cGMP or cAMP levels but reduced cGMP by maximally 2-fold over the first hour. This was also the case when phosphodiesterase-mediated cyclic nucleotide hydrolysis was inhibited by 3-isobutyl-1-methylxanthine, conditions in which efflux was maximal. These data indicate that MRP4 and MRP5 are low affinity cyclic nucleotide transporters that may at best function as overflow pumps, decreasing steep increases in cGMP levels under conditions where cGMP synthesis is strongly induced and phosphodiesterase activity is limiting.

Published

2003

8. Characterization of the transport of nucleoside analog drugs by the human multidrug resistance proteins MRP4 and MRP5.

Author

Reid G, Wielinga P, Zelcer N, De Haas M, Van Deemter L, Wijnholds J, Balzarini J, and Borst P

Subjects

Acrylates pharmacokinetics, Biological Transport, Cell Division drug effects, Cells, Cultured, Humans, Nucleosides pharmacology, Polymers pharmacokinetics, Multidrug Resistance-Associated Proteins metabolism, Nucleosides pharmacokinetics

Abstract

The human multidrug resistance proteins MRP4 and MRP5 are organic anion transporters that have the unusual ability to transport cyclic nucleotides and some nucleoside monophosphate analogs. Base and nucleoside analogs used in the chemotherapy of cancer and viral infections are potential substrates. To assess the possible contribution of MRP4 and MRP5 to resistance against these drugs, we have investigated the transport mediated by MRP4 and MRP5. In cytotoxicity assays, MRP4 conferred resistance to the antiviral agent 9-(2-phosphonomethoxyethyl)adenine (PMEA) and high-performance liquid chromatography analysis showed that, like MRP5, MRP4 transported PMEA in an unmodified form. MRP4 also mediated substantial resistance against other acyclic nucleoside phosphonates, whereas MRP5 did not. Apart from low-level MRP4-mediated cladribine resistance, the cytotoxicity of clinically used anticancer nucleosides was not influenced by overexpression of MRP4 or MRP5. In contrast, MRP5 mediated efflux of the pyrimidine-based antiviral 2',3'-dideoxynucleoside 2',3'-didehydro-2',3'-dideoxythymidine 5'-monophosphate (d4TMP) and its phosphoramidate derivative alaninyl-d4TMP from cells loaded with the 2',3'-didehydro-2',3'-dideoxythymidine prodrugs cyclosaligenyl-d4TMP and aryloxyphosphoramidate d4TMP (So324), respectively. Moreover, only inside-out membrane vesicles derived from MRP5-overexpressing cells accumulated alaninyl-d4TMP. Cellular efflux and vesicular uptake studies were carried out to further compare transport mediated by MRP4 and MRP5 and showed that dipyridamole, dilazep, nitrobenzyl mercaptopurine riboside, sildenafil, trequinsin and MK571 inhibited MRP4 more than MRP5, whereas cyclic nucleotides and monophosphorylated nucleoside analogs were equally poor inhibitors of both pumps. These results strongly suggest that the affinity of MRP4 and MRP5 for nucleotide-based substrates is low.

Published

2003

9. ABCC6/MRP6 mutations: further insight into the molecular pathology of pseudoxanthoma elasticum.

Author

Hu X, Plomp A, Wijnholds J, Ten Brink J, van Soest S, van den Born LI, Leys A, Peek R, de Jong PT, and Bergen AA

Subjects

Adult, Amino Acid Sequence, Child, DNA Mutational Analysis, DNA Primers, Gene Deletion, Gene Expression, Gene Frequency, Genetic Testing, Humans, Molecular Sequence Data, Pedigree, Protein Conformation, Reverse Transcriptase Polymerase Chain Reaction, Multidrug Resistance-Associated Proteins genetics, Mutation genetics, Pseudoxanthoma Elasticum genetics

Abstract

Pseudoxanthoma elasticum (PXE) is a hereditary disease characterized by progressive dystrophic mineralization of the elastic fibres. PXE patients frequently present with skin lesions and visual acuity loss. Recently, we and others showed that PXE is caused by mutations in the ABCC6/MRP6 gene. However, the molecular pathology of PXE is complicated by yet unknown factors causing the variable clinical expression of the disease. In addition, the presence of ABCC6/MRP6 pseudogenes and multiple ABCC6/MRP6-associated deletions complicate interpretation of molecular genetic studies. In this study, we present the mutation spectrum of ABCC6/MRP6 in 59 PXE patients from the Netherlands. We detected 17 different mutations in 65 alleles. The majority of mutations occurred in the NBF1 (nucleotide binding fold) domain, in the eighth cytoplasmatic loop between the 15th and 16th transmembrane regions, and in NBF2 of the predicted ABCC6/MRP6 protein. The R1141X mutation was by far the most common mutation identified in 19 (32.2%) patients. The second most frequent mutation, an intragenic deletion from exon 23 to exon 29 in ABCC6/MRP6, was detected in 11 (18.6%) of the patients. Our data include 11 novel ABCC6/MRP6 mutations, as well as additional segregation data relevant to the molecular pathology of PXE in a limited number of patients and families. The consequences of our data for the molecular pathology of PXE are discussed.

Published

2003

10. Thiopurine metabolism and identification of the thiopurine metabolites transported by MRP4 and MRP5 overexpressed in human embryonic kidney cells.

Author

Wielinga PR, Reid G, Challa EE, van der Heijden I, van Deemter L, de Haas M, Mol C, Kuil AJ, Groeneveld E, Schuetz JD, Brouwer C, De Abreu RA, Wijnholds J, Beijnen JH, and Borst P

Subjects

Biological Transport, Cells, Cultured, Chromatography, High Pressure Liquid, Drug Interactions, Humans, Kidney cytology, Kidney embryology, Kinetics, Mercaptopurine pharmacology, Methylthioinosine pharmacology, Multidrug Resistance-Associated Proteins biosynthesis, Ribosomal Proteins biosynthesis, Thioguanine pharmacology, Transfection, Mercaptopurine metabolism, Multidrug Resistance-Associated Proteins metabolism, Ribosomal Proteins metabolism, Thioguanine metabolism

Abstract

Mercaptopurines have been used as anticancer agents for more than 40 years, and most acute lymphoblastic leukemias are treated with 6-mercaptopurine (6MP) or 6-thioguanine (TG). Overexpression of the two related multidrug resistance proteins MRP4 and MRP5 has been shown to confer some resistance against mercaptopurines, which has been attributed to extrusion of mercaptopurine metabolites by these transporters. We have analyzed the mercaptopurine metabolites formed in human embryonic kidney cells and determined which metabolites are extruded by MRP4 and MRP5. Incubation with 6MP led to the formation of thioinosine and thioxanthosine metabolites and we found that thio-IMP was transported by both MRP4 and MRP5; MRP5 showed the highest transport rate. In contrast, only MRP5 transported thioxanthosine monophosphate (tXMP). During incubation with TG, the monophosphorylated form of thioguanosine was transported by both MRP4 and MRP5; the highest transport rate was for MRP4. Similarly, only 6-methyl-thio-IMP was formed during incubation with 6-methyl mercaptopurine riboside. This compound was a substrate for both MRP4 and MRP5; MRP4 showed the highest transport rate. Our results show that all major thiopurine monophosphates important in the efficacy of mercaptopurine treatment are transported by MRP4 and MRP5, although the substrate specificity of the two transporters differs in detail.

Published

2002

11. MRP6 (ABCC6) detection in normal human tissues and tumors.

Author

Scheffer GL, Hu X, Pijnenborg AC, Wijnholds J, Bergen AA, and Scheper RJ

Subjects

Animals, Antibodies, Monoclonal biosynthesis, Antibodies, Monoclonal immunology, Cell Line, Formaldehyde, Frozen Sections, Humans, Immunohistochemistry, Kidney chemistry, Liver chemistry, Multidrug Resistance-Associated Proteins analysis, Multidrug Resistance-Associated Proteins immunology, Neoplasms chemistry, Paraffin Embedding, Rats, Tissue Fixation, Drug Resistance, Multiple, Kidney metabolism, Liver metabolism, Multidrug Resistance-Associated Proteins metabolism, Neoplasms metabolism

Published

2002

12. Drug resistance caused by multidrug resistance-associated proteins.

Author

Wijnholds J

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 genetics, Animals, Biological Transport, Active, Biotransformation, Blood-Brain Barrier physiology, Blood-Testis Barrier physiology, Choroid Plexus metabolism, Drug Resistance, Multiple genetics, Female, Glutathione metabolism, Humans, Male, Mice, Multidrug Resistance-Associated Proteins genetics, Multigene Family, Nerve Tissue Proteins genetics, Nerve Tissue Proteins physiology, ATP Binding Cassette Transporter, Subfamily B, Member 1 physiology, Drug Resistance, Multiple physiology, Multidrug Resistance-Associated Proteins physiology

Abstract

Three types of drug efflux pumps, the multidrug resistance gene 1 (MDR1 or ABCB1)-encoded P glycoprotein, the multidrug resistance-associated protein (MRP or ABCC1) and breast cancer resistance protein (BCRP or ABCG2) may play an important part in the intrinsic or acquired defence of cells against drugs. Recent studies have begun to show the broad tissue distribution and drug substrate specificity of the seven MRP family members (MRP1-7; or ABCC1-6 and ABCC10). MRPs are (multispecific) organic anion transporters, which can transport negatively charged anionic drugs and neutral drugs conjugated to glutathione, glucuronate or sulfate. MRP4 and MRP5 broaden the spectrum of drug resistance to nucleotide analogue drugs. Some MRPs can also transport neutral drugs if co-transported with glutathione. MRP1 and MRP5 are abundant in almost every organ and are prominently present in the brain. High levels of MRP1 are present in the epithelium of the choroid plexus. Using mutant mice lacking a functional Mrp1 gene, we have previously shown the contribution of MRP1 to the blood-CSF (cerebrospinal fluid) drug permeability barrier. Recent studies indicate that the very low levels of MRP1 or MDR1 present in fibroblasts affect their sensitivity to a wide range of clinically important cytotoxic drugs. Even low concentrations of drug transporters may therefore protect cells against drugs.

Published

2002