Abstract
Intracellular infection and multi-organ colonization by the protozoan parasite, Trypanosoma cruzi, underlie the complex etiology of human Chagas disease. While T. cruzi can establish cytosolic residence in a broad range of mammalian cell types, the molecular mechanisms governing this process remain poorly understood. Despite the anticipated capacity for fatty acid synthesis in this parasite, recent observations suggest that intracellular T. cruzi amastigotes may rely on host fatty acid metabolism to support infection. To investigate this prediction, it was necessary to establish baseline lipidome information for the mammalian-infective stages of T. cruzi and their mammalian host cells. An unbiased, quantitative mass spectrometric analysis of lipid fractions was performed with the identification of 1079 lipids within 30 classes. From these profiles we deduced that T. cruzi amastigotes maintain an overall lipid identity that is distinguishable from mammalian host cells. A deeper analysis of the fatty acid moiety distributions within each lipid subclass facilitated the high confidence assignment of host- and parasite-like lipid signatures. This analysis unexpectedly revealed a strong host lipid signature in the parasite lipidome, most notably within its glycerolipid fraction. The near complete overlap of fatty acid moiety distributions observed for host and parasite triacylglycerols suggested that T. cruzi amastigotes acquired a significant portion of their lipidome from host triacylglycerol pools. Metabolic tracer studies confirmed long-chain fatty acid scavenging by intracellular T. cruzi amastigotes, a capacity that was significantly diminished in host cells deficient for de novo triacylglycerol synthesis via the diacylglycerol acyltransferases (DGAT1/2). Reduced T. cruzi amastigote proliferation in DGAT1/2-deficient fibroblasts further underscored the importance of parasite coupling to host triacylglycerol pools during the intracellular infection cycle. Thus, our comprehensive lipidomic dataset provides a substantially enhanced view of T. cruzi infection biology highlighting the interplay between host and parasite lipid metabolism with potential bearing on future therapeutic intervention strategies.
Highlights
Infection with the protozoan parasite Trypanosoma cruzi underlies the development of human Chagas disease, a progressive and debilitating condition characterized by cardiac and gastrointestinal disturbances [1]
The development of human Chagas disease is associated with persistent intracellular infection with the protozoan parasite, Trypanosoma cruzi, which displays tropism for tissues with characteristically high fatty acid flux, such as heart and adipose tissues
We provide several lines of evidence to demonstrate that cytosolically-localized T. cruzi amastigotes co-opt long chain fatty acids (LCFA), predominantly from host triacylglycerol (TG) pools, a process that facilitates the replication of this intracellular pathogen
Summary
Infection with the protozoan parasite Trypanosoma cruzi underlies the development of human Chagas disease, a progressive and debilitating condition characterized by cardiac and gastrointestinal disturbances [1]. Immune control mechanisms are insufficient to eliminate infection [8], leading to chronic infection with parasite persistence in a variety of tissues including cardiac muscle [9,10,11], gastrointestinal smooth muscle [7, 12, 13], and adipose tissue [7, 14, 15]. As such, understanding the mechanisms that underlie the successful intracellular colonization of diverse host cell types by T. cruzi is a crucial step to elucidating processes involved in the development and progression of both the acute and chronic stages of Chagas disease
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