Plasma Membrane-Located Purine Nucleotide Transport Proteins Are Key Components for Host Exploitation by Microsporidian Intracellular Parasites

Microsporidia are obligate intracellular parasites of most animal groups including humans, but despite their significant economic and medical importance there are major gaps in our understanding of how they exploit infected host cells. We have investigated the evolution, cellular locations and subst...

Descripción completa

Detalles Bibliográficos
Autores principales: Heinz, Eva, Hacker, Christian, Dean, Paul, Mifsud, John, Goldberg, Alina V., Williams, Tom A., Nakjang, Sirintra, Gregory, Alison, Hirt, Robert P., Lucocq, John M., Kunji, Edmund R. S., Embley, T. Martin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4256464/
https://www.ncbi.nlm.nih.gov/pubmed/25474405
http://dx.doi.org/10.1371/journal.ppat.1004547
_version_ 1782347589496078336
author Heinz, Eva
Hacker, Christian
Dean, Paul
Mifsud, John
Goldberg, Alina V.
Williams, Tom A.
Nakjang, Sirintra
Gregory, Alison
Hirt, Robert P.
Lucocq, John M.
Kunji, Edmund R. S.
Embley, T. Martin
author_facet Heinz, Eva
Hacker, Christian
Dean, Paul
Mifsud, John
Goldberg, Alina V.
Williams, Tom A.
Nakjang, Sirintra
Gregory, Alison
Hirt, Robert P.
Lucocq, John M.
Kunji, Edmund R. S.
Embley, T. Martin
author_sort Heinz, Eva
collection PubMed
description Microsporidia are obligate intracellular parasites of most animal groups including humans, but despite their significant economic and medical importance there are major gaps in our understanding of how they exploit infected host cells. We have investigated the evolution, cellular locations and substrate specificities of a family of nucleotide transport (NTT) proteins from Trachipleistophora hominis, a microsporidian isolated from an HIV/AIDS patient. Transport proteins are critical to microsporidian success because they compensate for the dramatic loss of metabolic pathways that is a hallmark of the group. Our data demonstrate that the use of plasma membrane-located nucleotide transport proteins (NTT) is a key strategy adopted by microsporidians to exploit host cells. Acquisition of an ancestral transporter gene at the base of the microsporidian radiation was followed by lineage-specific events of gene duplication, which in the case of T. hominis has generated four paralogous NTT transporters. All four T. hominis NTT proteins are located predominantly to the plasma membrane of replicating intracellular cells where they can mediate transport at the host-parasite interface. In contrast to published data for Encephalitozoon cuniculi, we found no evidence for the location for any of the T. hominis NTT transporters to its minimal mitochondria (mitosomes), consistent with lineage-specific differences in transporter and mitosome evolution. All of the T. hominis NTTs transported radiolabelled purine nucleotides (ATP, ADP, GTP and GDP) when expressed in Escherichia coli, but did not transport radiolabelled pyrimidine nucleotides. Genome analysis suggests that imported purine nucleotides could be used by T. hominis to make all of the critical purine-based building-blocks for DNA and RNA biosynthesis during parasite intracellular replication, as well as providing essential energy for parasite cellular metabolism and protein synthesis.
format Online
Article
Text
id pubmed-4256464
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-42564642014-12-11 Plasma Membrane-Located Purine Nucleotide Transport Proteins Are Key Components for Host Exploitation by Microsporidian Intracellular Parasites Heinz, Eva Hacker, Christian Dean, Paul Mifsud, John Goldberg, Alina V. Williams, Tom A. Nakjang, Sirintra Gregory, Alison Hirt, Robert P. Lucocq, John M. Kunji, Edmund R. S. Embley, T. Martin PLoS Pathog Research Article Microsporidia are obligate intracellular parasites of most animal groups including humans, but despite their significant economic and medical importance there are major gaps in our understanding of how they exploit infected host cells. We have investigated the evolution, cellular locations and substrate specificities of a family of nucleotide transport (NTT) proteins from Trachipleistophora hominis, a microsporidian isolated from an HIV/AIDS patient. Transport proteins are critical to microsporidian success because they compensate for the dramatic loss of metabolic pathways that is a hallmark of the group. Our data demonstrate that the use of plasma membrane-located nucleotide transport proteins (NTT) is a key strategy adopted by microsporidians to exploit host cells. Acquisition of an ancestral transporter gene at the base of the microsporidian radiation was followed by lineage-specific events of gene duplication, which in the case of T. hominis has generated four paralogous NTT transporters. All four T. hominis NTT proteins are located predominantly to the plasma membrane of replicating intracellular cells where they can mediate transport at the host-parasite interface. In contrast to published data for Encephalitozoon cuniculi, we found no evidence for the location for any of the T. hominis NTT transporters to its minimal mitochondria (mitosomes), consistent with lineage-specific differences in transporter and mitosome evolution. All of the T. hominis NTTs transported radiolabelled purine nucleotides (ATP, ADP, GTP and GDP) when expressed in Escherichia coli, but did not transport radiolabelled pyrimidine nucleotides. Genome analysis suggests that imported purine nucleotides could be used by T. hominis to make all of the critical purine-based building-blocks for DNA and RNA biosynthesis during parasite intracellular replication, as well as providing essential energy for parasite cellular metabolism and protein synthesis. Public Library of Science 2014-12-04 /pmc/articles/PMC4256464/ /pubmed/25474405 http://dx.doi.org/10.1371/journal.ppat.1004547 Text en © 2014 Embley et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Heinz, Eva
Hacker, Christian
Dean, Paul
Mifsud, John
Goldberg, Alina V.
Williams, Tom A.
Nakjang, Sirintra
Gregory, Alison
Hirt, Robert P.
Lucocq, John M.
Kunji, Edmund R. S.
Embley, T. Martin
Plasma Membrane-Located Purine Nucleotide Transport Proteins Are Key Components for Host Exploitation by Microsporidian Intracellular Parasites
title Plasma Membrane-Located Purine Nucleotide Transport Proteins Are Key Components for Host Exploitation by Microsporidian Intracellular Parasites
title_full Plasma Membrane-Located Purine Nucleotide Transport Proteins Are Key Components for Host Exploitation by Microsporidian Intracellular Parasites
title_fullStr Plasma Membrane-Located Purine Nucleotide Transport Proteins Are Key Components for Host Exploitation by Microsporidian Intracellular Parasites
title_full_unstemmed Plasma Membrane-Located Purine Nucleotide Transport Proteins Are Key Components for Host Exploitation by Microsporidian Intracellular Parasites
title_short Plasma Membrane-Located Purine Nucleotide Transport Proteins Are Key Components for Host Exploitation by Microsporidian Intracellular Parasites
title_sort plasma membrane-located purine nucleotide transport proteins are key components for host exploitation by microsporidian intracellular parasites
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4256464/
https://www.ncbi.nlm.nih.gov/pubmed/25474405
http://dx.doi.org/10.1371/journal.ppat.1004547
work_keys_str_mv AT heinzeva plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT hackerchristian plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT deanpaul plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT mifsudjohn plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT goldbergalinav plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT williamstoma plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT nakjangsirintra plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT gregoryalison plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT hirtrobertp plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT lucocqjohnm plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT kunjiedmundrs plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites
AT embleytmartin plasmamembranelocatedpurinenucleotidetransportproteinsarekeycomponentsforhostexploitationbymicrosporidianintracellularparasites

Ejemplares similares