A novel dense granule protein, GRA41, regulates timing of egress and calcium sensitivity in Toxoplasma gondii

Kaice A. LaFavers; Karla M. Márquez-Nogueras; Isabelle Coppens; Silvia N.J. Moreno; Gustavo Arrizabalaga

doi:10.1111/cmi.12749

A novel dense granule protein, GRA41, regulates timing of egress and calcium sensitivity in Toxoplasma gondii

Kaice A. LaFavers, Karla M. Márquez-Nogueras, Isabelle Coppens, Silvia N.J. Moreno, Gustavo Arrizabalaga

Bloomberg School of Public Health

Research output: Contribution to journal › Article › peer-review

14 Scopus citations

Abstract

Toxoplasma gondii is an obligate intracellular apicomplexan parasite with high seroprevalence in humans. Repeated lytic cycles of invasion, replication, and egress drive both the propagation and the virulence of this parasite. Key steps in this cycle, including invasion and egress, depend on tightly regulated calcium fluxes and, although many of the calcium-dependent effectors have been identified, the factors that detect and regulate the calcium fluxes are mostly unknown. To address this knowledge gap, we used a forward genetic approach to isolate mutants resistant to extracellular exposure to the calcium ionophore A23187. Through whole genome sequencing and complementation, we have determined that a nonsense mutation in a previously uncharacterised protein is responsible for the ionophore resistance of one of the mutants. The complete loss of this protein recapitulates the resistance phenotype and importantly shows defects in calcium regulation and in the timing of egress. The affected protein, GRA41, localises to the dense granules and is secreted into the parasitophorous vacuole where it associates with the tubulovesicular network. Our findings support a connection between the tubulovesicular network and ion homeostasis within the parasite, and thus a novel role for the vacuole of this important pathogen.

Original language	English (US)
Article number	e12749
Journal	Cellular microbiology
Volume	19
Issue number	9
DOIs	https://doi.org/10.1111/cmi.12749
State	Published - Sep 2017

Keywords

GRA41
Toxoplasma gondii
calcium
dense granule
egress
tubulovesicular network

ASJC Scopus subject areas

Microbiology
Immunology
Virology

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10.1111/cmi.12749

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title = "A novel dense granule protein, GRA41, regulates timing of egress and calcium sensitivity in Toxoplasma gondii",

abstract = "Toxoplasma gondii is an obligate intracellular apicomplexan parasite with high seroprevalence in humans. Repeated lytic cycles of invasion, replication, and egress drive both the propagation and the virulence of this parasite. Key steps in this cycle, including invasion and egress, depend on tightly regulated calcium fluxes and, although many of the calcium-dependent effectors have been identified, the factors that detect and regulate the calcium fluxes are mostly unknown. To address this knowledge gap, we used a forward genetic approach to isolate mutants resistant to extracellular exposure to the calcium ionophore A23187. Through whole genome sequencing and complementation, we have determined that a nonsense mutation in a previously uncharacterised protein is responsible for the ionophore resistance of one of the mutants. The complete loss of this protein recapitulates the resistance phenotype and importantly shows defects in calcium regulation and in the timing of egress. The affected protein, GRA41, localises to the dense granules and is secreted into the parasitophorous vacuole where it associates with the tubulovesicular network. Our findings support a connection between the tubulovesicular network and ion homeostasis within the parasite, and thus a novel role for the vacuole of this important pathogen.",

keywords = "GRA41, Toxoplasma gondii, calcium, dense granule, egress, tubulovesicular network",

author = "LaFavers, {Kaice A.} and M{\'a}rquez-Nogueras, {Karla M.} and Isabelle Coppens and Moreno, {Silvia N.J.} and Gustavo Arrizabalaga",

note = "Funding Information: We would like to thank Dr. Vern Carruthers for sharing the RhΔKu80 strain used for endogenous tagging and generation of the gra41 knockout as well as the gra2 knockout strains along with its parental and complemented strains and the MIC2 antibody, Dr. Peter Bradley for the GRA7 and ROP1 antibodies, Dr. Barry Stein for valuable training and advice in obtaining the transmission electron microscopy of the gra41 parental, knockout, and complemented strains, and Dr. Sanofar Abdeen for training and advice in recombinant protein purification. Also, we appreciate the intellectual input of Drs. Bill Sullivan, Rajshekhar Gaji, and Stacey Gilk into our work. We also like to thank all members of Arrizabalaga lab for critical reading of the manuscript. This research has been funded by NIH grants R21AI119516, R01AI123457, and RO3AI101624 to GA, AI110027, AI128356 and AI096836 to SNM, and AI060456 to KMN. KAL has been funded by an NIH training grant AI060519 and a fellowship from the American Heart Association 16PRE27260042. Publisher Copyright: {\textcopyright} 2017 John Wiley & Sons Ltd",

year = "2017",

month = sep,

doi = "10.1111/cmi.12749",

language = "English (US)",

volume = "19",

journal = "Cellular microbiology",

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AU - LaFavers, Kaice A.

AU - Márquez-Nogueras, Karla M.

AU - Coppens, Isabelle

AU - Moreno, Silvia N.J.

AU - Arrizabalaga, Gustavo

N1 - Funding Information: We would like to thank Dr. Vern Carruthers for sharing the RhΔKu80 strain used for endogenous tagging and generation of the gra41 knockout as well as the gra2 knockout strains along with its parental and complemented strains and the MIC2 antibody, Dr. Peter Bradley for the GRA7 and ROP1 antibodies, Dr. Barry Stein for valuable training and advice in obtaining the transmission electron microscopy of the gra41 parental, knockout, and complemented strains, and Dr. Sanofar Abdeen for training and advice in recombinant protein purification. Also, we appreciate the intellectual input of Drs. Bill Sullivan, Rajshekhar Gaji, and Stacey Gilk into our work. We also like to thank all members of Arrizabalaga lab for critical reading of the manuscript. This research has been funded by NIH grants R21AI119516, R01AI123457, and RO3AI101624 to GA, AI110027, AI128356 and AI096836 to SNM, and AI060456 to KMN. KAL has been funded by an NIH training grant AI060519 and a fellowship from the American Heart Association 16PRE27260042. Publisher Copyright: © 2017 John Wiley & Sons Ltd

PY - 2017/9

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N2 - Toxoplasma gondii is an obligate intracellular apicomplexan parasite with high seroprevalence in humans. Repeated lytic cycles of invasion, replication, and egress drive both the propagation and the virulence of this parasite. Key steps in this cycle, including invasion and egress, depend on tightly regulated calcium fluxes and, although many of the calcium-dependent effectors have been identified, the factors that detect and regulate the calcium fluxes are mostly unknown. To address this knowledge gap, we used a forward genetic approach to isolate mutants resistant to extracellular exposure to the calcium ionophore A23187. Through whole genome sequencing and complementation, we have determined that a nonsense mutation in a previously uncharacterised protein is responsible for the ionophore resistance of one of the mutants. The complete loss of this protein recapitulates the resistance phenotype and importantly shows defects in calcium regulation and in the timing of egress. The affected protein, GRA41, localises to the dense granules and is secreted into the parasitophorous vacuole where it associates with the tubulovesicular network. Our findings support a connection between the tubulovesicular network and ion homeostasis within the parasite, and thus a novel role for the vacuole of this important pathogen.

AB - Toxoplasma gondii is an obligate intracellular apicomplexan parasite with high seroprevalence in humans. Repeated lytic cycles of invasion, replication, and egress drive both the propagation and the virulence of this parasite. Key steps in this cycle, including invasion and egress, depend on tightly regulated calcium fluxes and, although many of the calcium-dependent effectors have been identified, the factors that detect and regulate the calcium fluxes are mostly unknown. To address this knowledge gap, we used a forward genetic approach to isolate mutants resistant to extracellular exposure to the calcium ionophore A23187. Through whole genome sequencing and complementation, we have determined that a nonsense mutation in a previously uncharacterised protein is responsible for the ionophore resistance of one of the mutants. The complete loss of this protein recapitulates the resistance phenotype and importantly shows defects in calcium regulation and in the timing of egress. The affected protein, GRA41, localises to the dense granules and is secreted into the parasitophorous vacuole where it associates with the tubulovesicular network. Our findings support a connection between the tubulovesicular network and ion homeostasis within the parasite, and thus a novel role for the vacuole of this important pathogen.

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KW - Toxoplasma gondii

KW - calcium

KW - dense granule

KW - egress

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DO - 10.1111/cmi.12749

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JF - Cellular microbiology

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ER -

A novel dense granule protein, GRA41, regulates timing of egress and calcium sensitivity in Toxoplasma gondii

Abstract

Keywords

ASJC Scopus subject areas

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