Literature DB >> 9294213

Isolation of a multispecific organic anion and cardiac glycoside transporter from rat brain.

B Noé1, B Hagenbuch, B Stieger, P J Meier.   

Abstract

A novel multispecific organic anion transporting polypeptide (oatp2) has been isolated from rat brain. The cloned cDNA contains 3,640 bp. The coding region extends over 1,983 nucleotides, thus encoding a polypeptide of 661 amino acids. Oatp2 is homologous to other members of the oatp gene family of membrane transporters with 12 predicted transmembrane domains, five potential glycosylation, and six potential protein kinase C phosphorylation sites. In functional expression studies in Xenopus laevis oocytes, oatp2 mediated uptake of the bile acids taurocholate (Km approximately 35 microM) and cholate (Km approximately 46 microM), the estrogen conjugates 17beta-estradiol-glucuronide (Km approximately 3 microM) and estrone-3-sulfate (Km approximately 11 microM), and the cardiac gylcosides ouabain (Km approximately 470 microM) and digoxin (Km approximately 0.24 microM). Although most of the tested compounds are common substrates of several oatp-related transporters, high-affinity uptake of digoxin is a unique feature of the newly cloned oatp2. On the basis of Northern blot analysis under high-stringency conditions, oatp2 is highly expressed in brain, liver, and kidney but not in heart, spleen, lung, skeletal muscle, and testes. These results provide further support for the overall significance of oatps as a new family of multispecific organic anion transporters. They indicate that oatp2 may play an especially important role in the brain accumulation and toxicity of digoxin and in the hepatobiliary and renal excretion of cardiac glycosides from the body.

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Year:  1997        PMID: 9294213      PMCID: PMC23365          DOI: 10.1073/pnas.94.19.10346

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  26 in total

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3.  Estradiol 17 beta-D-glucuronide is a high-affinity substrate for oatp organic anion transporter.

Authors:  N Kanai; R Lu; Y Bao; A W Wolkoff; M Vore; V L Schuster
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4.  Substantial excretion of digoxin via the intestinal mucosa and prevention of long-term digoxin accumulation in the brain by the mdr 1a P-glycoprotein.

Authors:  U Mayer; E Wagenaar; J H Beijnen; J W Smit; D K Meijer; J van Asperen; P Borst; A H Schinkel
Journal:  Br J Pharmacol       Date:  1996-11       Impact factor: 8.739

5.  Immunologic distribution of an organic anion transport protein in rat liver and kidney.

Authors:  A J Bergwerk; X Shi; A C Ford; N Kanai; E Jacquemin; R D Burk; S Bai; P M Novikoff; B Stieger; P J Meier; V L Schuster; A W Wolkoff
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6.  Molecular and functional characterization of an organic anion transporting polypeptide cloned from human liver.

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8.  Effect of antisense oligonucleotides on the expression of hepatocellular bile acid and organic anion uptake systems in Xenopus laevis oocytes.

Authors:  B Hagenbuch; B F Scharschmidt; P J Meier
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5.  An improved nonlinear model describing the hepatic pharmacokinetics of digoxin: evidence for two functionally different uptake systems and saturable binding.

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Review 8.  Active efflux across the blood-brain barrier: role of the solute carrier family.

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Review 10.  Pharmacogenetics of membrane transporters: an update on current approaches.

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