Dynamic RNA profiling in Plasmodium falciparum synchronized blood stages exposed to lethal doses of artesunate

BACKGROUND: Translation of the genome sequence of Plasmodium sp. into biologically relevant information relies on high through-put genomics technology which includes transcriptome analysis. However, few studies to date have used this powerful approach to explore transcriptome alterations of P. falci...

Descripción completa

Detalles Bibliográficos
Autores principales: Natalang, Onguma, Bischoff, Emmanuel, Deplaine, Guillaume, Proux, Caroline, Dillies, Marie-Agnès, Sismeiro, Odile, Guigon, Ghislaine, Bonnefoy, Serge, Patarapotikul, Jintana, Mercereau-Puijalon, Odile, Coppée, Jean-Yves, David, Peter H
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2536677/
https://www.ncbi.nlm.nih.gov/pubmed/18706115
http://dx.doi.org/10.1186/1471-2164-9-388
_version_ 1782159101622484992
author Natalang, Onguma
Bischoff, Emmanuel
Deplaine, Guillaume
Proux, Caroline
Dillies, Marie-Agnès
Sismeiro, Odile
Guigon, Ghislaine
Bonnefoy, Serge
Patarapotikul, Jintana
Mercereau-Puijalon, Odile
Coppée, Jean-Yves
David, Peter H
author_facet Natalang, Onguma
Bischoff, Emmanuel
Deplaine, Guillaume
Proux, Caroline
Dillies, Marie-Agnès
Sismeiro, Odile
Guigon, Ghislaine
Bonnefoy, Serge
Patarapotikul, Jintana
Mercereau-Puijalon, Odile
Coppée, Jean-Yves
David, Peter H
author_sort Natalang, Onguma
collection PubMed
description BACKGROUND: Translation of the genome sequence of Plasmodium sp. into biologically relevant information relies on high through-put genomics technology which includes transcriptome analysis. However, few studies to date have used this powerful approach to explore transcriptome alterations of P. falciparum parasites exposed to antimalarial drugs. RESULTS: The rapid action of artesunate allowed us to study dynamic changes of the parasite transcriptome in synchronous parasite cultures exposed to the drug for 90 minutes and 3 hours. Developmentally regulated genes were filtered out, leaving 398 genes which presented altered transcript levels reflecting drug-exposure. Few genes related to metabolic pathways, most encoded chaperones, transporters, kinases, Zn-finger proteins, transcription activating proteins, proteins involved in proteasome degradation, in oxidative stress and in cell cycle regulation. A positive bias was observed for over-expressed genes presenting a subtelomeric location, allelic polymorphism and encoding proteins with potential export sequences, which often belonged to subtelomeric multi-gene families. This pointed to the mobilization of processes shaping the interface between the parasite and its environment. In parallel, pathways were engaged which could lead to parasite death, such as interference with purine/pyrimidine metabolism, the mitochondrial electron transport chain, proteasome-dependent protein degradation or the integrity of the food vacuole. CONCLUSION: The high proportion of over-expressed genes encoding proteins exported from the parasite highlight the importance of extra-parasitic compartments as fields for exploration in drug research which, to date, has mostly focused on the parasite itself rather than on its intra and extra erythrocytic environment. Further work is needed to clarify which transcriptome alterations observed reflect a specific response to overcome artesunate toxicity or more general perturbations on the path to cellular death.
format Text
id pubmed-2536677
institution National Center for Biotechnology Information
language English
publishDate 2008
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-25366772008-09-16 Dynamic RNA profiling in Plasmodium falciparum synchronized blood stages exposed to lethal doses of artesunate Natalang, Onguma Bischoff, Emmanuel Deplaine, Guillaume Proux, Caroline Dillies, Marie-Agnès Sismeiro, Odile Guigon, Ghislaine Bonnefoy, Serge Patarapotikul, Jintana Mercereau-Puijalon, Odile Coppée, Jean-Yves David, Peter H BMC Genomics Research Article BACKGROUND: Translation of the genome sequence of Plasmodium sp. into biologically relevant information relies on high through-put genomics technology which includes transcriptome analysis. However, few studies to date have used this powerful approach to explore transcriptome alterations of P. falciparum parasites exposed to antimalarial drugs. RESULTS: The rapid action of artesunate allowed us to study dynamic changes of the parasite transcriptome in synchronous parasite cultures exposed to the drug for 90 minutes and 3 hours. Developmentally regulated genes were filtered out, leaving 398 genes which presented altered transcript levels reflecting drug-exposure. Few genes related to metabolic pathways, most encoded chaperones, transporters, kinases, Zn-finger proteins, transcription activating proteins, proteins involved in proteasome degradation, in oxidative stress and in cell cycle regulation. A positive bias was observed for over-expressed genes presenting a subtelomeric location, allelic polymorphism and encoding proteins with potential export sequences, which often belonged to subtelomeric multi-gene families. This pointed to the mobilization of processes shaping the interface between the parasite and its environment. In parallel, pathways were engaged which could lead to parasite death, such as interference with purine/pyrimidine metabolism, the mitochondrial electron transport chain, proteasome-dependent protein degradation or the integrity of the food vacuole. CONCLUSION: The high proportion of over-expressed genes encoding proteins exported from the parasite highlight the importance of extra-parasitic compartments as fields for exploration in drug research which, to date, has mostly focused on the parasite itself rather than on its intra and extra erythrocytic environment. Further work is needed to clarify which transcriptome alterations observed reflect a specific response to overcome artesunate toxicity or more general perturbations on the path to cellular death. BioMed Central 2008-08-18 /pmc/articles/PMC2536677/ /pubmed/18706115 http://dx.doi.org/10.1186/1471-2164-9-388 Text en Copyright © 2008 Natalang et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Natalang, Onguma
Bischoff, Emmanuel
Deplaine, Guillaume
Proux, Caroline
Dillies, Marie-Agnès
Sismeiro, Odile
Guigon, Ghislaine
Bonnefoy, Serge
Patarapotikul, Jintana
Mercereau-Puijalon, Odile
Coppée, Jean-Yves
David, Peter H
Dynamic RNA profiling in Plasmodium falciparum synchronized blood stages exposed to lethal doses of artesunate
title Dynamic RNA profiling in Plasmodium falciparum synchronized blood stages exposed to lethal doses of artesunate
title_full Dynamic RNA profiling in Plasmodium falciparum synchronized blood stages exposed to lethal doses of artesunate
title_fullStr Dynamic RNA profiling in Plasmodium falciparum synchronized blood stages exposed to lethal doses of artesunate
title_full_unstemmed Dynamic RNA profiling in Plasmodium falciparum synchronized blood stages exposed to lethal doses of artesunate
title_short Dynamic RNA profiling in Plasmodium falciparum synchronized blood stages exposed to lethal doses of artesunate
title_sort dynamic rna profiling in plasmodium falciparum synchronized blood stages exposed to lethal doses of artesunate
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2536677/
https://www.ncbi.nlm.nih.gov/pubmed/18706115
http://dx.doi.org/10.1186/1471-2164-9-388
work_keys_str_mv AT natalangonguma dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT bischoffemmanuel dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT deplaineguillaume dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT prouxcaroline dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT dilliesmarieagnes dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT sismeiroodile dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT guigonghislaine dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT bonnefoyserge dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT patarapotikuljintana dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT mercereaupuijalonodile dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT coppeejeanyves dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate
AT davidpeterh dynamicrnaprofilinginplasmodiumfalciparumsynchronizedbloodstagesexposedtolethaldosesofartesunate

Ejemplares similares