Metabolomic Analysis of Patient Plasma Yields Evidence of Plant-Like α-Linolenic Acid Metabolism in Plasmodium falciparum

V Lakshmanan, KY Rhee, W Wang, Y Yu… - The Journal of …, 2012 - academic.oup.com
V Lakshmanan, KY Rhee, W Wang, Y Yu, K Khafizov, A Fiser, P Wu, O Ndir, S Mboup…
The Journal of infectious diseases, 2012academic.oup.com
Metabolomics offers a powerful means to investigate human malaria parasite biology and
host-parasite interactions at the biochemical level, and to discover novel therapeutic targets
and biomarkers of infection. Here, we used an approach based on liquid chromatography
and mass spectrometry to perform an untargeted metabolomic analysis of metabolite
extracts from Plasmodium falciparum–infected and uninfected patient plasma samples, and
from an enriched population of in vitro cultured P. falciparum-infected and uninfected …
Abstract
Metabolomics offers a powerful means to investigate human malaria parasite biology and host-parasite interactions at the biochemical level, and to discover novel therapeutic targets and biomarkers of infection. Here, we used an approach based on liquid chromatography and mass spectrometry to perform an untargeted metabolomic analysis of metabolite extracts from Plasmodium falciparum–infected and uninfected patient plasma samples, and from an enriched population of in vitro cultured P. falciparum-infected and uninfected erythrocytes. Statistical modeling robustly segregated infected and uninfected samples based on metabolite species with significantly different abundances. Metabolites of the α-linolenic acid (ALA) pathway, known to exist in plants but not known to exist in P. falciparum until now, were enriched in infected plasma and erythrocyte samples. In vitro labeling with 13C-ALA showed evidence of plant-like ALA pathway intermediates in P. falciparum. Ortholog searches using ALA pathway enzyme sequences from 8 available plant genomes identified several genes in the P. falciparum genome that were predicted to potentially encode the corresponding enzymes in the hitherto unannotated P. falciparum pathway. These data suggest that our approach can be used to discover novel facets of host/malaria parasite biology in a high-throughput manner.
Oxford University Press
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