Functional specialization in nucleotide sugar transporters occurred through differentiation of the gene cluster EamA (DUF6) before the radiation of <it>Viridiplantae</it>

<p>Abstract</p> <p>Background</p> <p>The drug/metabolite transporter superfamily comprises a diversity of protein domain families with multiple functions including transport of nucleotide sugars. Drug/metabolite transporter domains are contained in both solute carrier f...

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Main Authors: Fredriksson Robert, Simmen Martin W, Almén Markus, Västermark Åke, Schiöth Helgi B
Format: Article
Language:English
Published: BMC 2011-05-01
Series:BMC Evolutionary Biology
Subjects:
Online Access:http://www.biomedcentral.com/1471-2148/11/123
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spelling doaj-1cfd16434c3e451f92fe34a6159017eb2021-09-02T06:20:31ZengBMCBMC Evolutionary Biology1471-21482011-05-0111112310.1186/1471-2148-11-123Functional specialization in nucleotide sugar transporters occurred through differentiation of the gene cluster EamA (DUF6) before the radiation of <it>Viridiplantae</it>Fredriksson RobertSimmen Martin WAlmén MarkusVästermark ÅkeSchiöth Helgi B<p>Abstract</p> <p>Background</p> <p>The drug/metabolite transporter superfamily comprises a diversity of protein domain families with multiple functions including transport of nucleotide sugars. Drug/metabolite transporter domains are contained in both solute carrier families 30, 35 and 39 proteins as well as in acyl-malonyl condensing enzyme proteins. In this paper, we present an evolutionary analysis of nucleotide sugar transporters in relation to the entire superfamily of drug/metabolite transporters that considers crucial intra-protein duplication events that have shaped the transporters. We use a method that combines the strengths of hidden Markov models and maximum likelihood to find relationships between drug/metabolite transporter families, and branches within families.</p> <p>Results</p> <p>We present evidence that the triose-phosphate transporters, domain unknown function 914, uracil-diphosphate glucose-N-acetylglucosamine, and nucleotide sugar transporter families have evolved from a domain duplication event before the radiation of <it>Viridiplantae </it>in the EamA family (previously called domain unknown function 6). We identify previously unknown branches in the solute carrier 30, 35 and 39 protein families that emerged simultaneously as key physiological developments after the radiation of <it>Viridiplantae</it>, including the "35C/E" branch of EamA, which formed in the lineage of <it>T. adhaerens </it>(<it>Animalia</it>). We identify a second cluster of DMTs, called the domain unknown function 1632 cluster, which has non-cytosolic N- and C-termini, and thus appears to have been formed from a different domain duplication event. We identify a previously uncharacterized motif, G-X(6)-G, which is overrepresented in the fifth transmembrane helix of C-terminal domains. We present evidence that the family called fatty acid elongases are homologous to transporters, not enzymes as had previously been thought.</p> <p>Conclusions</p> <p>The nucleotide sugar transporters families were formed through differentiation of the gene cluster EamA (domain unknown function 6) before <it>Viridiplantae</it>, showing for the first time the significance of EamA.</p> http://www.biomedcentral.com/1471-2148/11/123SLC30SLC35SLC39drug/metabolite transportersnucleotide sugar transportersEamAEmrEmulti drug resistance proteindual-topology proteinstransmembrane helix
collection DOAJ
language English
format Article
sources DOAJ
author Fredriksson Robert
Simmen Martin W
Almén Markus
Västermark Åke
Schiöth Helgi B
spellingShingle Fredriksson Robert
Simmen Martin W
Almén Markus
Västermark Åke
Schiöth Helgi B
Functional specialization in nucleotide sugar transporters occurred through differentiation of the gene cluster EamA (DUF6) before the radiation of <it>Viridiplantae</it>
BMC Evolutionary Biology
SLC30
SLC35
SLC39
drug/metabolite transporters
nucleotide sugar transporters
EamA
EmrE
multi drug resistance protein
dual-topology proteins
transmembrane helix
author_facet Fredriksson Robert
Simmen Martin W
Almén Markus
Västermark Åke
Schiöth Helgi B
author_sort Fredriksson Robert
title Functional specialization in nucleotide sugar transporters occurred through differentiation of the gene cluster EamA (DUF6) before the radiation of <it>Viridiplantae</it>
title_short Functional specialization in nucleotide sugar transporters occurred through differentiation of the gene cluster EamA (DUF6) before the radiation of <it>Viridiplantae</it>
title_full Functional specialization in nucleotide sugar transporters occurred through differentiation of the gene cluster EamA (DUF6) before the radiation of <it>Viridiplantae</it>
title_fullStr Functional specialization in nucleotide sugar transporters occurred through differentiation of the gene cluster EamA (DUF6) before the radiation of <it>Viridiplantae</it>
title_full_unstemmed Functional specialization in nucleotide sugar transporters occurred through differentiation of the gene cluster EamA (DUF6) before the radiation of <it>Viridiplantae</it>
title_sort functional specialization in nucleotide sugar transporters occurred through differentiation of the gene cluster eama (duf6) before the radiation of <it>viridiplantae</it>
publisher BMC
series BMC Evolutionary Biology
issn 1471-2148
publishDate 2011-05-01
description <p>Abstract</p> <p>Background</p> <p>The drug/metabolite transporter superfamily comprises a diversity of protein domain families with multiple functions including transport of nucleotide sugars. Drug/metabolite transporter domains are contained in both solute carrier families 30, 35 and 39 proteins as well as in acyl-malonyl condensing enzyme proteins. In this paper, we present an evolutionary analysis of nucleotide sugar transporters in relation to the entire superfamily of drug/metabolite transporters that considers crucial intra-protein duplication events that have shaped the transporters. We use a method that combines the strengths of hidden Markov models and maximum likelihood to find relationships between drug/metabolite transporter families, and branches within families.</p> <p>Results</p> <p>We present evidence that the triose-phosphate transporters, domain unknown function 914, uracil-diphosphate glucose-N-acetylglucosamine, and nucleotide sugar transporter families have evolved from a domain duplication event before the radiation of <it>Viridiplantae </it>in the EamA family (previously called domain unknown function 6). We identify previously unknown branches in the solute carrier 30, 35 and 39 protein families that emerged simultaneously as key physiological developments after the radiation of <it>Viridiplantae</it>, including the "35C/E" branch of EamA, which formed in the lineage of <it>T. adhaerens </it>(<it>Animalia</it>). We identify a second cluster of DMTs, called the domain unknown function 1632 cluster, which has non-cytosolic N- and C-termini, and thus appears to have been formed from a different domain duplication event. We identify a previously uncharacterized motif, G-X(6)-G, which is overrepresented in the fifth transmembrane helix of C-terminal domains. We present evidence that the family called fatty acid elongases are homologous to transporters, not enzymes as had previously been thought.</p> <p>Conclusions</p> <p>The nucleotide sugar transporters families were formed through differentiation of the gene cluster EamA (domain unknown function 6) before <it>Viridiplantae</it>, showing for the first time the significance of EamA.</p>
topic SLC30
SLC35
SLC39
drug/metabolite transporters
nucleotide sugar transporters
EamA
EmrE
multi drug resistance protein
dual-topology proteins
transmembrane helix
url http://www.biomedcentral.com/1471-2148/11/123
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