Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants

Malaria remains one of the most devastating parasitic diseases worldwide, with 90% of the malaria deaths in Africa in 2013 attributable to Plasmodium falciparum. The clinical symptoms of malaria include cycles of fever, corresponding to parasite rupture from red blood cells every 48 h. Parasite path...

Descripción completa

Detalles Bibliográficos
Autores principales: Thomas, Phaedra, Sedillo, Jennifer, Oberstaller, Jenna, Li, Suzanne, Zhang, Min, Singh, Naresh, Wang, Chengqi C. Q., Udenze, Kenneth, Jiang, Rays H. Y., Adams, John H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5082630/
https://www.ncbi.nlm.nih.gov/pubmed/27830190
http://dx.doi.org/10.1128/mSphere.00273-16
_version_ 1782463099398258688
author Thomas, Phaedra
Sedillo, Jennifer
Oberstaller, Jenna
Li, Suzanne
Zhang, Min
Singh, Naresh
Wang, Chengqi C. Q.
Udenze, Kenneth
Jiang, Rays H. Y.
Adams, John H.
author_facet Thomas, Phaedra
Sedillo, Jennifer
Oberstaller, Jenna
Li, Suzanne
Zhang, Min
Singh, Naresh
Wang, Chengqi C. Q.
Udenze, Kenneth
Jiang, Rays H. Y.
Adams, John H.
author_sort Thomas, Phaedra
collection PubMed
description Malaria remains one of the most devastating parasitic diseases worldwide, with 90% of the malaria deaths in Africa in 2013 attributable to Plasmodium falciparum. The clinical symptoms of malaria include cycles of fever, corresponding to parasite rupture from red blood cells every 48 h. Parasite pathways involved in the parasite’s ability to survive the host fever response, and indeed, the functions of ~40% of P. falciparum genes as a whole, are still largely unknown. Here, we evaluated the potential of scalable forward-genetic screening methods to identify genes involved in the host fever response. We performed a phenotypic screen for genes linked to the parasite response to febrile temperatures by utilizing a selection of single-disruption P. falciparum mutants generated via random piggyBac transposon mutagenesis in a previous study. We identified several mutants presenting significant phenotypes in febrile response screens compared to the wild type, indicating possible roles for the disrupted genes in this process. We present these initial studies as proof that forward genetics can be used to gain insight into critical factors associated with parasite biology. IMPORTANCE Though the P. falciparum genome sequence has been available for many years, ~40% of its genes do not have informative annotations, as they show no detectable homology to those of studied organisms. More still have not been evaluated via genetic methods. Scalable forward-genetic approaches that allow interrogation of gene function without any pre-existing knowledge are needed to hasten understanding of parasite biology, which will expedite the identification of drug targets and the development of future interventions in the face of spreading resistance to existing frontline drugs. In this work, we describe a new approach to pursue forward-genetic phenotypic screens for P. falciparum to identify factors associated with virulence. Future large-scale phenotypic screens developed to probe other such interesting phenomena, when considered in parallel, will prove a powerful tool for functional annotation of the P. falciparum genome, where so much remains undiscovered.
format Online
Article
Text
id pubmed-5082630
institution National Center for Biotechnology Information
language English
publishDate 2016
publisher American Society for Microbiology
record_format MEDLINE/PubMed
spelling pubmed-50826302016-11-09 Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants Thomas, Phaedra Sedillo, Jennifer Oberstaller, Jenna Li, Suzanne Zhang, Min Singh, Naresh Wang, Chengqi C. Q. Udenze, Kenneth Jiang, Rays H. Y. Adams, John H. mSphere Research Article Malaria remains one of the most devastating parasitic diseases worldwide, with 90% of the malaria deaths in Africa in 2013 attributable to Plasmodium falciparum. The clinical symptoms of malaria include cycles of fever, corresponding to parasite rupture from red blood cells every 48 h. Parasite pathways involved in the parasite’s ability to survive the host fever response, and indeed, the functions of ~40% of P. falciparum genes as a whole, are still largely unknown. Here, we evaluated the potential of scalable forward-genetic screening methods to identify genes involved in the host fever response. We performed a phenotypic screen for genes linked to the parasite response to febrile temperatures by utilizing a selection of single-disruption P. falciparum mutants generated via random piggyBac transposon mutagenesis in a previous study. We identified several mutants presenting significant phenotypes in febrile response screens compared to the wild type, indicating possible roles for the disrupted genes in this process. We present these initial studies as proof that forward genetics can be used to gain insight into critical factors associated with parasite biology. IMPORTANCE Though the P. falciparum genome sequence has been available for many years, ~40% of its genes do not have informative annotations, as they show no detectable homology to those of studied organisms. More still have not been evaluated via genetic methods. Scalable forward-genetic approaches that allow interrogation of gene function without any pre-existing knowledge are needed to hasten understanding of parasite biology, which will expedite the identification of drug targets and the development of future interventions in the face of spreading resistance to existing frontline drugs. In this work, we describe a new approach to pursue forward-genetic phenotypic screens for P. falciparum to identify factors associated with virulence. Future large-scale phenotypic screens developed to probe other such interesting phenomena, when considered in parallel, will prove a powerful tool for functional annotation of the P. falciparum genome, where so much remains undiscovered. American Society for Microbiology 2016-10-26 /pmc/articles/PMC5082630/ /pubmed/27830190 http://dx.doi.org/10.1128/mSphere.00273-16 Text en Copyright © 2016 Thomas et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (http://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Thomas, Phaedra
Sedillo, Jennifer
Oberstaller, Jenna
Li, Suzanne
Zhang, Min
Singh, Naresh
Wang, Chengqi C. Q.
Udenze, Kenneth
Jiang, Rays H. Y.
Adams, John H.
Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants
title Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants
title_full Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants
title_fullStr Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants
title_full_unstemmed Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants
title_short Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants
title_sort phenotypic screens identify parasite genetic factors associated with malarial fever response in plasmodium falciparum piggybac mutants
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5082630/
https://www.ncbi.nlm.nih.gov/pubmed/27830190
http://dx.doi.org/10.1128/mSphere.00273-16
work_keys_str_mv AT thomasphaedra phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants
AT sedillojennifer phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants
AT oberstallerjenna phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants
AT lisuzanne phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants
AT zhangmin phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants
AT singhnaresh phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants
AT wangchengqicq phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants
AT udenzekenneth phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants
AT jiangrayshy phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants
AT adamsjohnh phenotypicscreensidentifyparasitegeneticfactorsassociatedwithmalarialfeverresponseinplasmodiumfalciparumpiggybacmutants

Ejemplares similares