Novel slc22 transporter homologs in fly, worm, and human clarify the phylogeny of organic anion and cation transporters

doi:10.1152/physiolgenomics.00014.2004

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Physiol. Genomics 18: 12-24, 2004. First published March 30, 2004; doi:10.1152/physiolgenomics.00014.2004
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Received 20 January 2004; accepted in final form 26 March 2004.
Physiological Genomics 18:12-24 (2004)
1094-8341/04 $5.00 © 2004 American Physiological Society

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Comparative Genomics

Novel slc22 transporter homologs in fly, worm, and human clarify the phylogeny of organic anion and cation transporters

Satish A. Eraly¹, Julio C. Monte¹ and Sanjay K. Nigam¹^,2^,3

¹ Department of Medicine, University of California, San Diego, La Jolla, California 92093-0693
² Department of Pediatrics, University of California, San Diego, La Jolla, California 92093-0693
³ Department of Cellular Molecular Medicine, University of California, San Diego, La Jolla, California 92093-0693

Slc22 family organic anion and cation transporters (OATs, OCTs,and OCTNs) are transmembrane proteins expressed predominantlyin kidney and liver. These proteins mediate the uptake or excretionof numerous physiologically (and pharmacologically) importantcompounds, and accordingly have been the focus of intensivestudy. Here we investigate the molecular phylogeny of the slc22transporters, identifying homologs in Drosophila and C. elegans,several of which are developmentally regulated, as well as reportingthe cloning of a novel human family member, UST6, expressedexclusively in liver in both embryo and adult. The latter helpsdefine a subfamily within the OATs, which appears to have human-and rodent-specific members, raising potential issues with respectto the use of rodents as models for the transport of organicanions (which include many pharmaceuticals) in humans. Althoughthis phylogenetic inference could not be made on the basis ofsequence alignment, analysis of intron phasing suggests thatthe OAT, OCT, and OCTN lineages of the slc22 family formed afterthe divergence of vertebrates and invertebrates. Subsequently,these lineages expanded through independent tandem duplicationsto produce multiple gene pairs. After analyzing over 200 othertransporter genes, we find such pairing to be relatively specificto vertebrate organic anion and cation transporters, suggestingselection for gene pairing operating within this family in particular.This might reflect a requirement for redundancy or broader substratespecificity in vertebrates (compared to invertebrates), dueto their greater physiological complexity and thus potentiallybroader exposure to organic ions.

Drosophila; Caenorhabditis elegans; UST; SLC gene pairs

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