Gene expression signatures and small-molecule compounds link a protein kinase to Plasmodium falciparum motility

Kato, Nobutaka; Sakata, Taizo; Breton, Ghislaı̀n; Roch, Karine G. Le; Nagle, A. S.; Andersen, Carsten; Bursulaya, Badry; Henson, Kerstin; Johnson, Jeffrey R.; Kumar, Kota Arun; Marr, Felix; Mason, Daniel E.; McNamara, Case W.; Plouffe, David; Ramachandran, Vandana; Spooner, Muriel; Tuntland, Tove; Zhou, Yingyao; Peters, Eric C.; Chatterjee, Arnab K.; Schultz, Peter G.; Ward, Gary E.; Gray, Nathanael S.; Harper, Jeffrey F.; Winzeler, Elizabeth A.

doi:10.1038/nchembio.87

Cited by 205 publications

(249 citation statements)

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“…Furthermore, Go 6983, a PKC inhibitor (PfPKB catalytic domain is closely related to PKC) is able to affect in vitro recombinant PfPKB activity and reduce the ability of P. falciparum to invade erythrocytes (Kumar et al, 2004). Consistent with a vital role in parasite development, both PKB and CDPK1 are refractory to gene disruption in P. berghei and P. falciparum (Kato et al, 2008;Solyakov et al, 2011;Tewari et al, 2010). Using a broad-range serine/threonine kinase inhibitor (staurosporine), a marked reduction of phosphorylation of PfGAP45 was observed (Jones et al, 2009).…”

Section: Glideosome: Myosin Motor Assembly and Functionmentioning

confidence: 87%

“…Some of the predicted essential kinases were previously implicated in motility such as cAMPdependent protein kinase A (PKA) (Kurokawa et al, 2011;Leykauf et al, 2010), calcium-dependant protein kinase 1 (CDPK1) (Green et al, 2008;Kato et al, 2008;Winter et al, 2009), protein kinase B (PKB) (Vaid et al, 2008), and protein kinase G (PKG) (Hopp et al, 2012). These datasets therefore constitute an important resource for future hypotheses on the regulation of protein function by phosphorylation and their implications on host cell entry.…”

Section: Phosphoproteomementioning

confidence: 99%

“…In vitro phosphorylation assays of PfGAP45 and PfMTIP identified PfCDPK1 as a potential kinase (Green et al, 2008;Kato et al, 2008;Winter et al, 2009). PfCDPK1 is localized at the periphery of the P. falciparum merozoite and is therefore correctly positioned to fulfill such a function (Green et al, 2008).…”

Section: Glideosome: Myosin Motor Assembly and Functionmentioning

confidence: 99%

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Does protein phosphorylation govern host cell entry and egress by the Apicomplexa?

Jacot

Soldati‐Favre

2012

International Journal of Medical Microbiology

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a b s t r a c tMembers of the phylum Apicomplexa are responsible for a wide range of diseases in humans and animals. The absence of an effective vaccine or safe curing drugs and the continuous emergence of resistant parasites to available treatments impose a high demand on the identification of novel targets for intervention against the apicomplexans. Protein kinases are considered attractive potential therapeutic targets not only against cancers but also to combat infectious diseases. The scope and aim of this review is to report on the recent progress in dissecting the impact of protein phosphorylation in regulating motility and invasion.

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Section: Glideosome: Myosin Motor Assembly and Functionmentioning

confidence: 87%

Section: Phosphoproteomementioning

confidence: 99%

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Does protein phosphorylation govern host cell entry and egress by the Apicomplexa?

Jacot

Soldati‐Favre

2012

International Journal of Medical Microbiology

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“…GAP45 is known to be phosphorylated by at least two different kinases, CDPK1 and PKB (Green et al, 2008) (Vaid et al, 2008). MTIP is also phosphorylated by CDPK1 (Kato et al, 2008) (Green et al, 2008) and recently it has been shown in T. gondii that dephosphorylation of GAP45 is a prerequisite for its association with MTIP (Gilk et al, 2009). Thus, phosphorylation/dephosphorylation appears to have a role in controlling motor function.…”

Section: -Biological Processes From a Signalling Perspectivementioning

confidence: 99%

“…The best defined function of Ca 2+ as a second messenger come from studies utilizing transgenic parasites expressing a Ca 2+ reporter in P. berghei gametocytes in which cytosolic Ca 2+ mobilization occurs within seconds once cells are exposed to conditions encountered in the mosquito midgut and is critical for the initiation of gametogenesis (Billker et al, 2004 et al, 2004). PfCDPK1 was originally suggested to be exported to the parasitophorous vacuole in a myristoylation/palmitoylation-dependent manner (Moskes et al, 2004) but more recent studies suggest that it is associated with the parasite plasma membrane and has a role in merozoite egress and invasion (Green et al, 2008;Kato et al, 2008 (Green et al, 2008) and PKB phosphorylates GAP45 (Vaid et al, 2008). Clearly, Ca 2+ -dependent pathways need to be dissected to provide insights of molecular mechanisms underlying parasite development.…”

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confidence: 99%

Signalling in malaria parasites – The MALSIG consortium

et al. 2009

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Summary :Depending on their developmental stage in the life cycle, malaria parasites develop within or outside host cells, and in extremely diverse contexts such as the vertebrate liver and blood circulation, or the insect midgut and hemocoel. Cellular and molecular mechanisms enabling the parasite to sense and respond to the intra-and the extra-cellular environments are therefore key elements for the proliferation and transmission of Plasmodium, and therefore are, from a public health perspective, strategic targets in the fight against this deadly disease. The MALSIG consortium, which was initiated in February 2009, was designed with the primary objective to integrate research ongoing in Europe and India on i) the properties of Plasmodium signalling molecules, and ii) developmental processes occurring at various points of the parasite life cycle. On one hand, functional studies of individual genes and their products in Plasmodium falciparum (and in the technically more manageable rodent model Plasmodium berghei) are providing information on parasite protein kinases and phosphatases, and of the molecules governing cyclic nucleotide metabolism and calcium signalling. On the other hand, cellular and molecular studies are elucidating key steps of parasite development such as merozoite invasion and egress in blood and liver parasite stages, control of DNA replication in asexual and sexual development, membrane dynamics and trafficking, production of gametocytes in the vertebrate host and further parasite development in the mosquito. This article, which synthetically reviews such signalling molecules

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