Proteins and lipids of glycosomal membranes from Leishmania tarentolae and Trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]

Proteins and lipids of glycosomal membranes from Leishmania tarentolae and Trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]

In kinetoplastid protists, several metabolic pathways, including glycolysis and purine salvage, are located in glycosomes, which are microbodies that are evolutionarily related to peroxisomes. With the exception of some potential transporters for fatty acids, and one member of the mitochondrial carr...

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Main Authors: Claudia Colasante, Frank Voncken, Theresa Manful, Thomas Ruppert, Aloysius G M Tielens, Jaap J van Hellemond, Christine Clayton
Format: Article
Language:English
Published: F1000 Research Ltd 2013-01-01
Series:F1000Research
Subjects:
Protein Chemistry & Proteomics
Online Access:http://f1000research.com/articles/2-27/v1
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spelling doaj-99f8fa655d134e6c898214bb02e674432020-11-25T03:24:41ZengF1000 Research LtdF1000Research2046-14022013-01-01210.12688/f1000research.2-27.v11189Proteins and lipids of glycosomal membranes from Leishmania tarentolae and Trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]Claudia Colasante0Frank Voncken1Theresa Manful2Thomas Ruppert3Aloysius G M Tielens4Jaap J van Hellemond5Christine Clayton6Institut für Anatomie und Zellbiologie, Giessen, 35392, GermanyDepartment of Biological Sciences and Hull York Medical School, University of Hull, Hull, HU6 7RX, UKDepartment of Biochemistry, Cell & Molecular Biology, University of Ghana, Accra, P.O. Box LG 54, GhanaDKFZ-ZMBH Alliance, Zentrum für Molekulare Biologie der Universität Heidelberg, Heidelberg, D69120, GermanyDepartment of Biochemistry and Cell Biology, Faculty of Veterinary Medicine, Utrecht University, Utrecht, PO Box 80176, NetherlandsDepartment of Medical Microbiology and Infectious Diseases, ErasmusMC University Medical Center, Rotterdam, PO box 2040, NetherlandsDKFZ-ZMBH Alliance, Zentrum für Molekulare Biologie der Universität Heidelberg, Heidelberg, D69120, GermanyIn kinetoplastid protists, several metabolic pathways, including glycolysis and purine salvage, are located in glycosomes, which are microbodies that are evolutionarily related to peroxisomes. With the exception of some potential transporters for fatty acids, and one member of the mitochondrial carrier protein family, proteins that transport metabolites across the glycosomal membrane have yet to be identified. We show here that the phosphatidylcholine species composition of Trypanosoma brucei glycosomal membranes resembles that of other cellular membranes, which means that glycosomal membranes are expected to be impermeable to small hydrophilic molecules unless transport is facilitated by specialized membrane proteins. Further, we identified 464 proteins in a glycosomal membrane preparation from Leishmania tarentolae. The proteins included approximately 40 glycosomal matrix proteins, and homologues of peroxisomal membrane proteins - PEX11, GIM5A and GIM5B; PXMP4, PEX2 and PEX16 - as well as the transporters GAT1 and GAT3. There were 27 other proteins that could not be unambiguously assigned to other compartments, and that had predicted trans-membrane domains. However, no clear candidates for transport of the major substrates and intermediates of energy metabolism were found. We suggest that, instead, these metabolites are transported via pores formed by the known glycosomal membrane proteins.http://f1000research.com/articles/2-27/v1Protein Chemistry & Proteomics
collection DOAJ
language English
format Article
sources DOAJ
author Claudia Colasante
Frank Voncken
Theresa Manful
Thomas Ruppert
Aloysius G M Tielens
Jaap J van Hellemond
Christine Clayton
spellingShingle Claudia Colasante
Frank Voncken
Theresa Manful
Thomas Ruppert
Aloysius G M Tielens
Jaap J van Hellemond
Christine Clayton
Proteins and lipids of glycosomal membranes from Leishmania tarentolae and Trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]
F1000Research
Protein Chemistry & Proteomics
author_facet Claudia Colasante
Frank Voncken
Theresa Manful
Thomas Ruppert
Aloysius G M Tielens
Jaap J van Hellemond
Christine Clayton
author_sort Claudia Colasante
title Proteins and lipids of glycosomal membranes from Leishmania tarentolae and Trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]
title_short Proteins and lipids of glycosomal membranes from Leishmania tarentolae and Trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]
title_full Proteins and lipids of glycosomal membranes from Leishmania tarentolae and Trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]
title_fullStr Proteins and lipids of glycosomal membranes from Leishmania tarentolae and Trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]
title_full_unstemmed Proteins and lipids of glycosomal membranes from Leishmania tarentolae and Trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]
title_sort proteins and lipids of glycosomal membranes from leishmania tarentolae and trypanosoma brucei [v1; ref status: indexed, http://f1000r.es/x1]
publisher F1000 Research Ltd
series F1000Research
issn 2046-1402
publishDate 2013-01-01
description In kinetoplastid protists, several metabolic pathways, including glycolysis and purine salvage, are located in glycosomes, which are microbodies that are evolutionarily related to peroxisomes. With the exception of some potential transporters for fatty acids, and one member of the mitochondrial carrier protein family, proteins that transport metabolites across the glycosomal membrane have yet to be identified. We show here that the phosphatidylcholine species composition of Trypanosoma brucei glycosomal membranes resembles that of other cellular membranes, which means that glycosomal membranes are expected to be impermeable to small hydrophilic molecules unless transport is facilitated by specialized membrane proteins. Further, we identified 464 proteins in a glycosomal membrane preparation from Leishmania tarentolae. The proteins included approximately 40 glycosomal matrix proteins, and homologues of peroxisomal membrane proteins - PEX11, GIM5A and GIM5B; PXMP4, PEX2 and PEX16 - as well as the transporters GAT1 and GAT3. There were 27 other proteins that could not be unambiguously assigned to other compartments, and that had predicted trans-membrane domains. However, no clear candidates for transport of the major substrates and intermediates of energy metabolism were found. We suggest that, instead, these metabolites are transported via pores formed by the known glycosomal membrane proteins.
topic Protein Chemistry & Proteomics
url http://f1000research.com/articles/2-27/v1
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