Literature DB >> 12590146

Cloning and characterization of a novel Na+-dependent glucose transporter (NaGLT1) in rat kidney.

Naoshi Horiba1, Satohiro Masuda, Ayako Takeuchi, Daisuke Takeuchi, Masahiro Okuda, Ken-ichi Inui.   

Abstract

To identify novel transporters in the kidney, we have constructed an mRNA data base composed of 1000 overall clones by random sequencing of a male rat kidney cDNA library. After a BLAST search, approximately 40% of the clones were unknown and/or unannotated and were screened by measuring the uptake of various compounds using Xenopus oocytes. One clone stimulated the uptake of alpha-methyl-d-glucopyranoside and therefore was termed rat Na(+)-dependent glucose transporter 1 (rNaGLT1). The rNaGLT1 cDNA (2173 bp) has an open reading frame encoding a 484-amino acid protein, showing <22% homology to known SGLT and GLUT glucose transporters. alpha-Methyl-d-glucopyranoside uptake by rNaGLT1 cRNA-injected oocytes showed saturability, with an apparent K(m) of 3.7 mm and a coupling ratio of 1:1 with Na(+). rNaGLT1 mRNA was expressed predominantly in the kidney upon Northern blot analysis and reverse transcription-PCR. Reverse transcription-PCR in microdissected nephron segments revealed that rNaGLT1 mRNA was primarily localized in the proximal tubules. A clear signal corresponding to rNaGLT1 protein was recognized in the brush-border (but not basolateral) membrane fraction by immunoblot analysis. The rNaGLT1 mRNA level in the kidney was significantly higher than rat SGLT1 and SGLT2 mRNA levels. These findings suggest that rNaGLT1 is a novel Na(+)-dependent glucose transporter with low substrate affinity that mediates tubular reabsorption of glucose.

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Year:  2003        PMID: 12590146     DOI: 10.1074/jbc.M212240200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  16 in total

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4.  Alternative channels for urea in the inner medulla of the rat kidney.

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Authors:  Marina Subramaniam; Lynn P Weber; Matthew E Loewen
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Review 9.  Sodium-glucose cotransporter-2 inhibitors: Understanding the mechanisms for therapeutic promise and persisting risks.

Authors:  Rachel J Perry; Gerald I Shulman
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10.  Increase in SGLT1-mediated transport explains renal glucose reabsorption during genetic and pharmacological SGLT2 inhibition in euglycemia.

Authors:  Timo Rieg; Takahiro Masuda; Maria Gerasimova; Eric Mayoux; Kenneth Platt; David R Powell; Scott C Thomson; Hermann Koepsell; Volker Vallon
Journal:  Am J Physiol Renal Physiol       Date:  2013-11-13
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