Comparative proteomics uncovers low asparagine content in Plasmodium tRip‐KO proteins

Author:

Pitolli Martina1,Cela Marta1,Kapps Delphine1,Chicher Johana2,Despons Laurence1,Frugier Magali1ORCID

Affiliation:

1. Université de Strasbourg, CNRS, Architecture et Réactivité de l'ARN Strasbourg France

2. Strasbourg‐Esplanade Proteomics Facility Université de Strasbourg Strasbourg France

Abstract

AbstracttRNAs 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.

Funder

Laboratoire d'Excellence NetRNA

Equipex

Fondation pour la Recherche Médicale

Publisher

Wiley

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