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1 Department of Medical Genetics, Biomedicum Helsinki, and 4 Finnish Genome Center, University of Helsinki, 00014 Helsinki, Finland; 2 Department I of Medicine, Eberhard-Karls University, Tübingen, Germany; 3 Department of Physiology and Pharmacology, School of Biomedical Sciences, University of Queensland, Brisbane, Queensland 4072, Australia; and 5 Department of Biosciences, Novum, Karolinska Institute, 14157 Huddinge, Sweden
The solute carrier gene family SLC26
consists of tissue-specific anion exchanger genes, three of them
associated with distinct human recessive disorders. By a genome-driven
approach, several new SLC26 family members have been identified,
including a kidney- and pancreas-specific gene, SLC26A6. We report the
functional characterization of SLC26A6 and two new alternatively
spliced variants, named SLC26A6c and SLC26A6d. Immunofluorescence
studies on transiently transfected cells indicated membrane
localization and indicated that both NH2- and COOH-terminal
tails of the SLC26A6 variants are located intracellularly, suggesting a
topology with an even number of transmembrane domains. Functional
expression of the three proteins in Xenopus oocytes
demonstrated Cl
and SO

was inhibited by DIDS and HCO
alternative splicing; PDZ domain; SLC26
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