Host reticulocytes provide metabolic reservoirs that can be exploited by malaria parasites

Srivastava, A; Creek, DJ; Evans, KJ; De Souza, D; Schofield, L; Muller, S; Barrett, MP; McConville, MJ; Waters, AP

Author(s): Srivastava, A; Creek, DJ; Evans, KJ; De Souza, D; Schofield, L; Muller, S; Barrett, MP; McConville, MJ; Waters, AP;
Details: Publication Year 2015-06,Volume 11,Issue #6,Page e1004882
Journal Title: PLoS Pathogens
Publication Type: Journal Article
Abstract: Human malaria parasites proliferate in different erythroid cell types during infection. Whilst Plasmodium vivax exhibits a strong preference for immature reticulocytes, the more pathogenic P. falciparum primarily infects mature erythrocytes. In order to assess if these two cell types offer different growth conditions and relate them to parasite preference, we compared the metabolomes of human and rodent reticulocytes with those of their mature erythrocyte counterparts. Reticulocytes were found to have a more complex, enriched metabolic profile than mature erythrocytes and a higher level of metabolic overlap between reticulocyte resident parasite stages and their host cell. This redundancy was assessed by generating a panel of mutants of the rodent malaria parasite P. berghei with defects in intermediary carbon metabolism (ICM) and pyrimidine biosynthesis known to be important for P. falciparum growth and survival in vitro in mature erythrocytes. P. berghei ICM mutants (pbpepc-, phosphoenolpyruvate carboxylase and pbmdh-, malate dehydrogenase) multiplied in reticulocytes and committed to sexual development like wild type parasites. However, P. berghei pyrimidine biosynthesis mutants (pboprt-, orotate phosphoribosyltransferase and pbompdc-, orotidine 5'-monophosphate decarboxylase) were restricted to growth in the youngest forms of reticulocytes and had a severe slow growth phenotype in part resulting from reduced merozoite production. The pbpepc-, pboprt- and pbompdc- mutants retained virulence in mice implying that malaria parasites can partially salvage pyrimidines but failed to complete differentiation to various stages in mosquitoes. These findings suggest that species-specific differences in Plasmodium host cell tropism result in marked differences in the necessity for parasite intrinsic metabolism. These data have implications for drug design when targeting mature erythrocyte or reticulocyte resident parasites.
Publisher: PLOS
Research Division(s): Population Health And Immunity
PubMed ID: 26042734
Publisher's Version: https://doi.org/10.1371/journal.ppat.1004882
Open Access at Publisher's Site: http://journals.plos.org/plospathogens/article?id=10.1371/journal.ppat.1004882
Terms of Use/Rights Notice: Refer to copyright notice on published article.

Creation Date: 2015-06-15 09:53:29

Last Modified: 2019-04-01 09:07:47