Lipidomics and anti‐trypanosomatid chemotherapy

Biagiotti, Michael; Dominguez, Sedelia; Yamout, Nader; Zufferey, Rachel

doi:10.1186/s40169-017-0160-7

Cited by 21 publications

(25 citation statements)

References 96 publications

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“…Remarkably in protozoan parasites such as Plasmodium falciparum and Trypanosoma brucei, the Kennedy pathway has already been proposed as a potentially relevant drug target [42][43][44][45][46][47][48]. Further investigation of the Kennedy metabolic pathway in S. mansoni could be important for drug discovery and drug repositioning (i.e.…”

Section: Plos Neglected Tropical Diseasesmentioning

confidence: 99%

Drug effects on metabolic profiles of Schistosoma mansoni adult male parasites detected by 1H-NMR spectroscopy

et al. 2020

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Schistosomiasis is one of the most devastating neglected tropical parasitic diseases caused by trematodes of the genus Schistosoma. Praziquantel (PZQ) is today the only drug used in humans and animals for the treatment of schistosomiasis but unfortunately it is poorly effective on larval and juvenile stages of the parasite. Therefore, it is urgent the discovery of new drug targets and compounds. We have recently showed that the anti-anginal drug perhexiline maleate (PHX) is very active on multiple developmental stages of Schistosoma mansoni in vitro. It is well known that PHX impacts the lipid metabolism in mammals, but the final target on schistosomes still remains unknown. The aim of this study was to evaluate the ability of 1 H nuclear magnetic resonance (NMR) spectroscopy in revealing metabolic perturbations due to PHX treatment of S. mansoni adult male worms. The effects of PHX were compared with the ones induced by vehicle and gambogic acid, in order to detect different metabolic profiles and specificity of the PHX action. Remarkably a list of metabolites associated to PHX-treatment was identified with enrichment in several connected metabolic pathways including also the Kennedy pathway mediating the glycerophospholipid metabolism. Our study represents the first 1 H-NMR metabolomic approach to characterize the response of S. mansoni to drug treatment. The obtained "metabolic fingerprint" associated to PHX treatment could represent a strategy for displaying cellular metabolic changes for any given drug and to compare compounds targeting similar or distinct biochemical pathways.

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Section: Plos Neglected Tropical Diseasesmentioning

confidence: 99%

Drug effects on metabolic profiles of Schistosoma mansoni adult male parasites detected by 1H-NMR spectroscopy

et al. 2020

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“…In a similar approach, a lipidomic analysis of the T. brucei procyclic (the parasite form transmitted by the tsetse fly) versus the mammalian bloodstream forms revealed significant differences in sphingolipid metabolism. While the relevance of such observation awaits clarification, the absence of some of these sphingolipid species in vertebrates strengthens the importance of such lipids in parasite biology (reviewed in Biagiotti et al, 2017). The metabolome of T. brucei procyclic forms was further analyzed by Kamleh et al, 2008, in which the authors compared the procyclic forms fed on glucose (the main carbon source) versus proline (highly abundant in the tsetse fly), providing evidence that metabolic alterations are a significant part of the parasite's adaptation to the tsetse vector.…”

Section: Sensing Each Othermentioning

confidence: 99%

“…Plasmodium, for example, has lost the ability to synthesize de novo amino acids (aa) and has devised mechanisms to scavenge aa from the catabolism of hemoglobin (Gardner et al, 2002;Olszewski et al, 2009). Trypanosoma cruzi, which completely lacks the ability to synthesize cholesterol like most parasites (reviewed in Biagiotti et al, 2017), has developed efficient ways of taking up and storing host cholesterol (Pereira et al, 2011).…”

Section: Sensing Each Othermentioning

confidence: 99%

Parasite Sensing of Host Nutrients and Environmental Cues

Zuzarte‐Luís

Mota

2018

Cell Host & Microbe

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Parasites undergo complex life cycles that comprise a wide variety of cellular differentiation events in different host compartments and transmission across multiple hosts. As parasites depend on host resources, it is not surprising they have developed efficient mechanisms to sense alterations and adapt to the available resources in a wide range of environments. Here we provide an overview of the nutritional needs of different parasites throughout their diverse life stages and highlight recent insights into strategies that both hosts and parasites have developed to meet these nutritional requirements needed for defense, survival, and replication. These studies will provide the foundation for a systems-level understanding of host-parasite interactions, which will require the integration of molecular, epidemiologic, and mechanistic data and the application of interdisciplinary approaches to model parasite regulatory networks that are triggered by alterations in host resources.

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“…In fact omics-based analyses have facilitated the broadening of R&D researches in the field of drug development. Lipidomics analyses have yielded the characterization of lipid structures, protein lipidation pathways in post-translational modifications, and their putative functions for kinetoplastid parasites ( 33 , 34 ). This knowledge will allow the search for new classes of anti-parasitic pharmaceuticals.…”

Section: Trends In Drug Development For Kinetoplastid Infectionsmentioning

confidence: 99%

Human Kinetoplastid Protozoan Infections: Where Are We Going Next?

et al. 2018

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Kinetoplastida trypanosomatidae microorganisms are protozoan parasites exhibiting a developmental stage in the gut of insect vectors and tissues of vertebrate hosts. During the vertebrate infective stages, these parasites alter the differential expression of virulence genes, modifying their biological and antigenic properties in order to subvert the host protective immune responses and establish a persistent infection. One of the hallmarks of kinetoplastid parasites is their evasion mechanisms from host immunity, leading to disease chronification. The diseases caused by kinetoplastid parasites are neglected by the global expenditures in research and development, affecting millions of individuals in the low and middle-income countries located mainly in the tropical and subtropical regions. However, investments made by public and private initiatives have over the past decade leveraged important lines of intervention that if well-integrated to health care programs will likely accelerate disease control initiatives. This review summarizes recent advances in public health care principles, including new drug discoveries and their rational use with chemotherapeutic vaccines, and the implementation of control efforts to spatially mapping the kinetoplastid infections through monitoring of infected individuals in epidemic areas. These approaches should bring us the means to track genetic variation of parasites and drug resistance, integrating this knowledge into effective stewardship programs to prevent vector-borne kinetoplastid infections in areas at risk of disease spreading.

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Lipidomics and anti‐trypanosomatid chemotherapy

Cited by 21 publications

References 96 publications

Drug effects on metabolic profiles of Schistosoma mansoni adult male parasites detected by 1H-NMR spectroscopy

Drug effects on metabolic profiles of Schistosoma mansoni adult male parasites detected by 1H-NMR spectroscopy

Parasite Sensing of Host Nutrients and Environmental Cues

Human Kinetoplastid Protozoan Infections: Where Are We Going Next?

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