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The systematic functional analysis of Plasmodium protein kinases identifies essential regulators of mosquito transmission.

Cell host & microbe | 2010

Although eukaryotic protein kinases (ePKs) contribute to many cellular processes, only three Plasmodium falciparum ePKs have thus far been identified as essential for parasite asexual blood stage development. To identify pathways essential for parasite transmission between their mammalian host and mosquito vector, we undertook a systematic functional analysis of ePKs in the genetically tractable rodent parasite Plasmodium berghei. Modeling domain signatures of conventional ePKs identified 66 putative Plasmodium ePKs. Kinomes are highly conserved between Plasmodium species. Using reverse genetics, we show that 23 ePKs are redundant for asexual erythrocytic parasite development in mice. Phenotyping mutants at four life cycle stages in Anopheles stephensi mosquitoes revealed functional clusters of kinases required for sexual development and sporogony. Roles for a putative SR protein kinase (SRPK) in microgamete formation, a conserved regulator of clathrin uncoating (GAK) in ookinete formation, and a likely regulator of energy metabolism (SNF1/KIN) in sporozoite development were identified.

Pubmed ID: 20951971 RIS Download

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Associated grants

  • Agency: Medical Research Council, United Kingdom
    Id: G0900109
  • Agency: Medical Research Council, United Kingdom
    Id: G0501670
  • Agency: Wellcome Trust, United Kingdom
    Id: 087656
  • Agency: Wellcome Trust, United Kingdom
    Id: WT078335MA
  • Agency: Wellcome Trust, United Kingdom
    Id: WT089085/Z/09/Z
  • Agency: Wellcome Trust, United Kingdom

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BALB/cAnNCrl (tool)

RRID:MGI:2683685

laboratory mouse with name BALB/cAnNCrl from MGI.

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C57BL/6J (tool)

RRID:IMSR_JAX:000664

Mus musculus with name C57BL/6J from IMSR.

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