Novel roles of dense granule protein 12 (GRA12) in<i>Toxoplasma gondii</i>infection

Wang, Jin‐Lei; Bai, Meng-Jie; Elsheikha, Hany M.; Liang, Qin‐Li; Li, Tingting; Cao, Xue-Zhen; Zhu, Xing‐Quan

doi:10.1096/fj.201901416rr

Cited by 34 publications

(62 citation statements)

References 58 publications

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“…Intriguingly, the phosphorylation level of GRA2 was detected to be up-regulated significantly in the comparison group of PE vs. JI, which suggested that phosphorylation may be one of the important mechanisms in mediating the function of GRA2. Surprisingly, both GRA3 and GRA12 were identified with enhanced phosphorylation level in this study yet were shown to be dispensable for the lytic cycle of T. gondii in vitro, however, they play essential roles in acute infection of T. gondii in vivo (Craver and Knoll, 2007;Rommereim et al, 2016;Fox et al, 2019;Wang et al, 2020). The explanation of this discrepancy may be that GRA3 and GRA12 do not play their roles independently in the lytic cycle process of tachyzoites but interdependently, just as other GRA proteins (Rommereim et al, 2016).…”

Section: Discussioncontrasting

confidence: 54%

iTRAQ-Based Phosphoproteomic Analysis of Toxoplasma gondii Tachyzoites Provides Insight Into the Role of Phosphorylation for its Invasion and Egress

Pan

et al. 2020

Front. Cell. Infect. Microbiol.

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The invasion and egress are two key steps in lytic cycle vital to the propagation of Toxoplasma gondii infection, and phosphorylation is believed to play important roles in these processes. However, the phosphoproteome of T. gondii at these two stages has not been characterized. In this study, we profiled the phosphoproteome of tachyzoites at the stages of “just invading” (JI) and “prior to egress” (PE) based on iTRAQ quantitative analysis, in which a total of 46 phosphopeptides, 42 phosphorylation sites, and 38 phosphoproteins were detected. In the comparison of PE vs. JI, 10 phosphoproteins were detected with their phosphorylation level significantly changed, and four of them were demonstrated to be significantly down-regulated at the transcriptional level. Bioinformatic analysis of these identified phosphoproteins suggested that phosphorylation-mediated modulation of protein function was employed to regulate the pathway of toxoplasmosis and metabolism and cellular processes correlated with tachyzoite’s binding, location, and metabolism, and thus play vital roles in the parasite lytic cycle. Moreover, cytoskeletal network (CN)-associated Inner Membrane Complex (IMC1, IMC4, IMC6 and IMC12), Intravascular Network (IVN)-related GRAs (GRA2, GRA3, GRA7 and GRA12), and Parasitophorous Vacuole Membrane (PVM)-localized ROP5 were shown to be enriched at the central nodes in the protein interaction network generated by bioinformatic analysis, in which the phosphorylation level of IMC4, GRA2, GRA3, and GRA12 were found to be significantly regulated. This study revealed the main cellular processes and key phosphoproteins crucial for the invasion and egress of T. gondii, which will provide new insights into the developmental biology of T. gondii in vitro and contribute to the understanding of pathogen-host interaction from the parasite perspective.

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Section: Discussioncontrasting

confidence: 54%

iTRAQ-Based Phosphoproteomic Analysis of Toxoplasma gondii Tachyzoites Provides Insight Into the Role of Phosphorylation for its Invasion and Egress

Pan

et al. 2020

Front. Cell. Infect. Microbiol.

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“…To achieve this, each mouse was infected i.p. with 10 3 tachyzoites (five mice/strain), and five days later, the parasite burden in the peritoneal fluid was examined by plaque assay as described previously [22]. Briefly, mice were humanely sacrificed, and peritoneal cells were harvested by lavage with phosphate buffered saline (PBS) containing 1% FBS.…”

Section: Optimization Of the Vaccination Dosementioning

confidence: 99%

“…Then 100 µL freshly liberated parasites were used to infect confluent HFF monolayers maintained in RPMI1640 medium for seven days. Then, T. gondii-infected HFFs were fixed and stained, and the sizes and numbers of plaques formed by the growing tachyzoites were determined using the plaque assay as described previously [22].…”

Section: Optimization Of the Vaccination Dosementioning

confidence: 99%

RHΔgra17Δnpt1 Strain of Toxoplasma gondii Elicits Protective Immunity Against Acute, Chronic and Congenital Toxoplasmosis in Mice

et al. 2020

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In the present study, a dense granule protein 17 (gra17) and novel putative transporter (npt1) double deletion mutant of Toxoplasma gondii RH strain was engineered. The protective efficacy of vaccination using RHΔgra17Δnpt1 tachyzoites against acute, chronic, and congenital toxoplasmosis was studied in a mouse model. Immunization using RHΔgra17Δnpt1 induced a strong humoral and cellular response, as indicated by the increased levels of anti-T. gondii specific IgG, interleukin 2 (IL-2), IL-10, IL-12, and interferon-gamma (IFN-γ). Vaccinated mice were protected against a lethal challenge dose (103 tachyzoites) of wild-type homologous (RH) strain and heterologous (PYS and TgC7) strains, as well as against 100 tissue cysts or oocysts of Pru strain. Vaccination also conferred protection against chronic infection with 10 tissue cysts or oocysts of Pru strain, where the numbers of brain cysts in the vaccinated mice were significantly reduced compared to those detected in the control (unvaccinated + infected) mice. In addition, vaccination protected against congenital infection with 10 T. gondii Pru oocysts (administered orally on day 5 of gestation) as shown by the increased litter size, survival rate and the bodyweight of pups born to vaccinated dams compared to those born to unvaccinated + infected dams. The brain cyst burden of vaccinated dams was significantly lower than that of unvaccinated dams infected with oocysts. Our data show that T. gondii RHΔgra17Δnpt1 mutant strain can protect mice against acute, chronic, and congenital toxoplasmosis by balancing inflammatory response with immunogenicity.

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“…Corticosteroid (dexamethasone) immune suppressed or IFN‐γ −/− mice infected with parasites lacking GRA12 I/II succumb to infection. Despite its implication in modulation of IFN‐γ mediated immune responses, the GTPase effectors do not assemble on the vacuoles of parasites without GRA12 (Fox et al, 2019; Wang et al, 2020). GRA7/II together with other PVM associated GRAs were found to make up the cyst wall and membrane and shown to be important for cyst formation (Guevara, Fox, & Bzik, 2020).…”

Section: Discussionmentioning

confidence: 99%

“…Once phosphorylated, IRGs are unable to hydrolyse GTP and cannot form oligomers, hence IRG loading onto the PVM is disabled (Steinfeldt et al, 2010). GRA12, on the other hand, resides within the PV and contributes to both parasite virulence and establishment of chronic infection through modulation of IFN‐γ mediated immune responses without involving the GTPase effectors (Fox et al, 2019; Wang et al, 2020).…”

Section: Introductionmentioning

confidence: 99%

Toxoplasma gondii GRA60 is an effector protein that modulates host cell autonomous immunity and contributes to virulence

Nyonda

Hammoudi

et al. 2020

Cellular Microbiology

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Toxoplasma gondii infects virtually any nucleated cell and resides inside a non‐phagocytic vacuole surrounded by a parasitophorous vacuolar membrane (PVM). Pivotal to the restriction of T. gondii dissemination upon infection in murine cells is the recruitment of immunity regulated GTPases (IRGs) and guanylate binding proteins (GBPs) to the PVM that leads to pathogen elimination. The virulent T. gondii type I RH strain secretes a handful of effectors including the dense granule protein GRA7, the serine–threonine kinases ROP17 and ROP18, and a pseudo‐kinase ROP5, that synergistically inhibit the recruitment of IRGs to the PVM. Here, we characterise GRA60, a novel dense granule effector, which localises to the vacuolar space and PVM and contributes to virulence of RH in mice, suggesting a role in the subversion of host cell defence mechanisms. Members of the host cell IRG defence system Irgb10 and Irga6 are recruited to the PVM of RH parasites lacking GRA60 as observed previously for the avirulent RHΔrop5 mutant, with RH preventing such recruitment. Deletion of GRA60 in RHΔrop5 leads to a recruitment of IRGs comparable to the single knockouts. GRA60 therefore represents a novel parasite effector conferring resistance to IRGs in type I parasites, and found associated to ROP18, a member of the virulence complex.

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Novel roles of dense granule protein 12 (GRA12) inToxoplasma gondiiinfection

Cited by 34 publications

References 58 publications

iTRAQ-Based Phosphoproteomic Analysis of Toxoplasma gondii Tachyzoites Provides Insight Into the Role of Phosphorylation for its Invasion and Egress

iTRAQ-Based Phosphoproteomic Analysis of Toxoplasma gondii Tachyzoites Provides Insight Into the Role of Phosphorylation for its Invasion and Egress

RHΔgra17Δnpt1 Strain of Toxoplasma gondii Elicits Protective Immunity Against Acute, Chronic and Congenital Toxoplasmosis in Mice

Toxoplasma gondii GRA60 is an effector protein that modulates host cell autonomous immunity and contributes to virulence

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