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Comparative proteomics uncovers low asparagine content in Plasmodium tRip-KO proteins.

Martina PitolliMarta CelaDelphine KappsJohana ChicherLaurence DesponsMagali Frugier
Published in: IUBMB life (2024)
tRNAs are not only essential for decoding the genetic code, but their abundance also has a strong impact on the rate of protein production, folding, and on the stability of the translated messenger RNAs. Plasmodium expresses a unique surface protein called tRip, involved in the import of exogenous tRNAs into the parasite. Comparative proteomic analysis of the blood stage of wild-type and tRip-KO variant of P. berghei parasites revealed that downregulated proteins in the mutant parasite are distinguished by a bias in their asparagine content. Furthermore, the demonstration of the possibility of charging host tRNAs with Plasmodium aminoacyl-tRNA synthetases led us to propose that imported host tRNAs participate in parasite protein synthesis. These results also suggest a novel mechanism of translational control in which import of host tRNAs emerge as regulators of gene expression in the Plasmodium developmental cycle and pathogenesis, by enabling the synthesis of asparagine-rich regulatory proteins that efficiently and selectively control the parasite infectivity.
Keyphrases
  • plasmodium falciparum
  • wild type
  • gene expression
  • transcription factor
  • dna methylation
  • protein protein
  • mass spectrometry
  • single cell
  • genome wide
  • molecular dynamics simulations
  • small molecule