Identifying host regulators and inhibitors of liver stage malaria infection using kinase activity profiles

Arang, Nadia; Kain, Heather S.; Glennon, Elizabeth K.K.; Bello, Thomas R.; Dudgeon, Denali R.; Walter, Emily N. F.; Gujral, Taranjit S.; Kaushansky, Alexis

doi:10.1038/s41467-017-01345-2

Cited by 40 publications

(55 citation statements)

References 46 publications

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“…Optimal maintenance of LS infection is dependent on the activity of a large number of host kinases regulating processes such as cytoskeletal organization and apoptosis (Arang et al, 2017). These observations are consistent with the hypothesis that the parasite rewires a portion of host cell signaling in a manner that disrupts canonical signal transduction cascades.…”

Section: Resultsmentioning

confidence: 99%

“…Once a parasite is inside a hepatocyte, its survival is also influenced by host cell factors, including levels of the tumor suppressor p53 (Douglass et al, 2015; Kaushansky et al, 2013), the degree of endoplasmic reticulum (ER) stress (Inácio et al, 2015; Kaushansky and Kappe, 2015), and regulation of an extensive network of kinases (Arang et al, 2017; Prudêncio et al, 2008; Ruivo et al, 2016). Interestingly, a large portion of the hepatocyte kinome regulates LS infection (Arang et al, 2017), suggesting that phosphosignaling in the cell might be globally altered in the context of infection. Consistent with this hypothesis, a variety of signaling pathways are disrupted by Plasmodium infection on the transcriptional, protein, and post-translational levels (Albuquerque et al, 2009; Kaushansky et al, 2013; Posfai et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

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Alterations in Phosphorylation of Hepatocyte Ribosomal Protein S6 Control Plasmodium Liver Stage Infection

et al. 2019

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SUMMARY Plasmodium parasites are highly selective when infecting hepatocytes and induce many changes within the host cell upon infection. While several host cell factors have been identified that are important for liver infection, our understanding of what facilitates the maintenance of infection remains incomplete. Here, we describe a role for phosphorylated ribosomal protein S6 (Ser235/236) (p-RPS6) in Plasmodium yoelii-infected hepatocytes. Blocking RPS6 phosphorylation prior to infection decreases the number of liver stage parasites within 24 h. Infected hepatocytes exhibit elevated levels of p-RPS6 while simultaneously abrogating the induction of phosphorylation of RPS6 in response to insulin stimulation. This is in contrast with the regulation of p-RPS6 by Toxoplasma gondii, which elevates levels of p-RPS6 after infection but does not alter the response to insulin. Our data support a model in which RPS6 phosphorylation is uncoupled from canonical regulators in Plasmodium-infected hepatocytes and is relied on by the parasite to maintain infection.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Alterations in Phosphorylation of Hepatocyte Ribosomal Protein S6 Control Plasmodium Liver Stage Infection

et al. 2019

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“…FGFR4 has previously been implicated in liver stage development of P. yoelii in Hepa1-6 cells, as one among a number of ‘hits’ in a screen investigating the role of host kinases in EEF development. [25], although negative results were obtained in a similar screen investigating P. berghei [26].…”

Section: Resultsmentioning

confidence: 99%

“…The possibility that interactions between Pf34 and FGFR4 could contribute to a functionally-important invasion complex is supported by FGFR4’s role in liver-specific signalling pathways, and evidence of reduced EEF formation in the absence of FGFR4 [24, 25, 29]. Investigation of the effect of disruption of these interactions upon sporozoite invasion is a priority.…”

Section: Discussionmentioning

confidence: 99%

A screen forPlasmodium falciparumsporozoite surface protein binding to human hepatocyte surface receptors identifies novel host-pathogen interactions

Segireddy

Dundas

Knoeckel

et al. 2020

Preprint

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Sporozoite invasion of hepatocytes is a necessary step prior to development of malaria, with similarities, at the cellular level, to merozoite invasion of erythrocytes. In the case of the malaria blood-stage, efforts to identify host-pathogen protein-protein interactions have yielded important insights including vaccine candidates. In the case of sporozoite-hepatocyte invasion, the host-pathogen protein-protein interactions involved are poorly understood. Here, we performed a systematic screen to identify such interactions. We substantially extended previous Plasmodium falciparum and human surface protein ectodomain libraries, creating new libraries containing 88 P. falciparum sporozoite protein coding sequences and 182 sequences encoding human hepatocyte surface proteins. Having expressed recombinant proteins from these sequences, we used a plate-based assay capable of detecting low affinity interactions between recombinant proteins, modified for enhanced throughput, to screen the proteins for interactions. We were able to test 7540 sporozoite-hepatocyte protein pairs under conditions likely to be sensitive for interaction. We report and characterise an interaction between human fibroblast growth factor receptor 4 (FGFR4) and the P. falciparum protein Pf34, and describe an additional interaction between human low-density lipoprotein receptor (LDLR) and the P. falciparum protein PIESP15. Strategies to inhibit these interactions may have value in malaria prevention, and the modified interaction screening assay and protein expression libraries we report may be of wider value to the community.

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“…S6). Neither Erastin nor Sorafenib impacted the growth of Plasmodium-infected erythrocytes 21 , further minimizing the likelihood that these drugs directly target parasite pathways ( Fig. S5b).…”

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confidence: 99%

Ferroptosis-like signaling facilitates a potent innate defense againstPlasmodiuminfection

Arang

Glennon

et al. 2018

Preprint

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The facets of host control during Plasmodium liver infection remain largely unknown and conventional innate regulatory pathways are only minimally effective at eliminating parasites1-3. Ferroptosis, a recently described form of iron-dependent cell death that drives accumulation of reactive oxygen species and lipid peroxides, but has not yet been shown to function as an innate immune response4,5. Inducing ferroptosis with pharmacologicals or by genetic perturbation of its negative regulators, GPX4 and SLC7a11, dramatically reduces survival of the Plasmodium Liver Stage. In contrast, knockdown or knockout of NOX1 or knockdown of TFR1, which are required for ferroptosis, increases the number of Liver Stage parasites. Moreover, we demonstrate that blocking ferroptosis renders parasite-infected hepatocytes resistant to P53-mediated hepatocyte death. Our work establishes that ferroptotic signaling serves to control Plasmodium infection in the liver and raises the possibility that ferroptosis operates as an axis of the innate immune system to defend against intracellular pathogens.

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Identifying host regulators and inhibitors of liver stage malaria infection using kinase activity profiles

Cited by 40 publications

References 46 publications

Alterations in Phosphorylation of Hepatocyte Ribosomal Protein S6 Control Plasmodium Liver Stage Infection

Alterations in Phosphorylation of Hepatocyte Ribosomal Protein S6 Control Plasmodium Liver Stage Infection

A screen forPlasmodium falciparumsporozoite surface protein binding to human hepatocyte surface receptors identifies novel host-pathogen interactions

Ferroptosis-like signaling facilitates a potent innate defense againstPlasmodiuminfection

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