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CRISPR-based functional profiling of the Toxoplasma gondii genome during acute murine infection.

Christopher J GiulianoKenneth J WeiFaye M HarlingBenjamin S WaldmanMadeline A FarringerElizabeth A BoydstonTammy C T LanRaina W ThomasAlice L HerneisenAllen G SanderlinIsabelle CoppensJeffrey D DvorinSebastian Lourido
Published in: Nature microbiology (2024)
Examining host-pathogen interactions in animals can capture aspects of infection that are obscured in cell culture. Using CRISPR-based screens, we functionally profile the entire genome of the apicomplexan parasite Toxoplasma gondii during murine infection. Barcoded gRNAs enabled bottleneck detection and mapping of population structures within parasite lineages. Over 300 genes with previously unknown roles in infection were found to modulate parasite fitness in mice. Candidates span multiple axes of host-parasite interaction. Rhoptry Apical Surface Protein 1 was characterized as a mediator of host-cell tropism that facilitates repeated invasion attempts. GTP cyclohydrolase I was also required for fitness in mice and druggable through a repurposed compound, 2,4-diamino-6-hydroxypyrimidine. This compound synergized with pyrimethamine against T. gondii and malaria-causing Plasmodium falciparum parasites. This work represents a complete survey of an apicomplexan genome during infection of an animal host and points to novel interfaces of host-parasite interaction.
Keyphrases
  • plasmodium falciparum
  • toxoplasma gondii
  • genome wide
  • physical activity
  • single cell
  • high resolution
  • dna methylation
  • cross sectional
  • skeletal muscle
  • trypanosoma cruzi
  • gene expression
  • high density