Gamma-glutamylcysteine synthetase and tryparedoxin 1 exert high control on the antioxidant system in Trypanosoma cruzi contributing to drug resistance and infectivity

González-Chávez, Zabdi; Vázquez, Citlali; Mejia-Tlachi, Marlen; Márquez-Dueñas, Claudia; Manning‐Cela, Rebeca; Encalada, Rusely; Rodrı́guez-Enrı́quez, Sara; Michels, Paul A.M.; Moreno‐Sánchez, Rafael; Saavedra, Emma

doi:10.1016/j.redox.2019.101231

Cited by 24 publications

(24 citation statements)

References 60 publications

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“…After 13 days of interaction, almost all the cells have been infected. From these results, we concluded that the fraction of infected cells after 18 h of the initial cell-parasite interaction can be used as an estimate for the parasite invasion efficiency, in agreement with former results 12,[18][19][20] .…”

Section: Resultssupporting

confidence: 90%

Motility patterns of Trypanosoma cruzi trypomastigotes correlate with the efficiency of parasite invasion in vitro

Arias-del-Angel

Santana-Solano

Santillán

et al. 2020

Sci Rep

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Numerous works have demonstrated that trypanosomatid motility is relevant for parasite replication and sensitivity. Nonetheless, although some findings indirectly suggest that motility also plays an important role during infection, this has not been extensively investigated. This work is aimed at partially filling this void for the case of Trypanosoma cruzi. After recording swimming T. cruzi trypomastigotes (CL Brener strain) and recovering their individual trajectories, we statistically analyzed parasite motility patterns. We did this with parasites that swim alone or above monolayer cultures of different cell lines. Our results indicate that T. cruzi trypomastigotes change their motility patterns when they are in the presence of mammalian cells, in a cell-line dependent manner. We further performed infection experiments in which each of the mammalian cell cultures were incubated for 2 h together with trypomastigotes, and measured the corresponding invasion efficiency. Not only this parameter varied from cell line to cell line, but it resulted to be positively correlated with the corresponding intensity of the motility pattern changes. Together, these results suggest that T. cruzi trypomastigotes are capable of sensing the presence of mammalian cells and of changing their motility patterns accordingly, and that this might increase their invasion efficiency.

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Section: Resultssupporting

confidence: 90%

Motility patterns of Trypanosoma cruzi trypomastigotes correlate with the efficiency of parasite invasion in vitro

Arias-del-Angel

Santana-Solano

Santillán

et al. 2020

Sci Rep

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“…Finally, GBD had an IC 50 = 66 ± 12 μM. For comparison, under similar exposure protocols, the IC 50 for benznidazole was 12 ± 2 μM [ 35 ] whereas for NFX the value was 3 ± 0.6 μM (Aketzalli Silva Carmona & Emma Saavedra, unpublished results). In addition, the compounds were evaluated on human foreskin fibroblasts (HFF1) to measure cytotoxicity; the effects on these cells are summarized in Table 4 .…”

Section: Resultsmentioning

confidence: 99%

Computational Drug Repositioning for Chagas Disease Using Protein-Ligand Interaction Profiling

Juárez-Saldívar

Schroeder

Salentin

et al. 2020

IJMS

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Chagas disease, caused by Trypanosoma cruzi (T. cruzi), affects nearly eight million people worldwide. There are currently only limited treatment options, which cause several side effects and have drug resistance. Thus, there is a great need for a novel, improved Chagas treatment. Bifunctional enzyme dihydrofolate reductase-thymidylate synthase (DHFR-TS) has emerged as a promising pharmacological target. Moreover, some human dihydrofolate reductase (HsDHFR) inhibitors such as trimetrexate also inhibit T. cruzi DHFR-TS (TcDHFR-TS). These compounds serve as a starting point and a reference in a screening campaign to search for new TcDHFR-TS inhibitors. In this paper, a novel virtual screening approach was developed that combines classical docking with protein-ligand interaction profiling to identify drug repositioning opportunities against T. cruzi infection. In this approach, some food and drug administration (FDA)-approved drugs that were predicted to bind with high affinity to TcDHFR-TS and whose predicted molecular interactions are conserved among known inhibitors were selected. Overall, ten putative TcDHFR-TS inhibitors were identified. These exhibited a similar interaction profile and a higher computed binding affinity, compared to trimetrexate. Nilotinib, glipizide, glyburide and gliquidone were tested on T. cruzi epimastigotes and showed growth inhibitory activity in the micromolar range. Therefore, these compounds could lead to the development of new treatment options for Chagas disease.

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“…Despite the established relationship between melarsoprol and trypanothione, the specific mode of melarsoprol cell killing remains unknown (24). Because the biosynthetic and redox utilization pathways contain enzymes unique to Trypanosomatids, they have been broadly explored as drug targets against American trypanosomes and Leishmania species (15,(28)(29)(30)(31)(32).…”

Section: Traditional Methods Of Overexpression Library Formation By Cmentioning

confidence: 99%

“…6). The essential gene encoding gglutamylcysteine synthetase (GSH1, Tb927.10.12370)(41), which is the rate-limiting step of trypanothione biosynthesis(28,32,33,42), was 191-fold overrepresented in melarsoprol survivors(TABLE 2). Overexpression of GSH1 in T. brucei and other Trypanosomatids increases the concentration of intracellular trypanothione and has been shown to promote melarsoprol resistance under laboratory conditions(33).…”

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confidence: 99%

ATrypanosoma bruceiORFeome-based Gain-of-Function Library identifies genes that promote survival during melarsoprol treatment

Carter

Gomez

Gritz

et al. 2020

Preprint

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Trypanosoma brucei is an early branching protozoan parasite that causes human and animal African Trypanosomiasis. Forward genetics approaches are powerful tools for uncovering novel aspects of Trypanosomatid biology, pathogenesis, and therapeutic approaches against trypanosomiasis. Here we have generated a T. brucei cloned ORFeome consisting of over 90% of the targeted 7,245 genes and used it to make an inducible Gain-of-Function parasite library broadly applicable to large-scale forward genetic screens. We conducted a proof of principle genetic screen to identify genes whose expression promotes survival in melarsoprol, a critical drug of last resort. The 57 genes identified as overrepresented in melarsoprol survivor populations included the rate-limiting enzyme for the biosynthesis of an established drug target (trypanothione), validating the tool. In addition, novel genes associated with gene expression, flagellum localization, and mitochondrion localization were identified and a subset of those genes increased melarsoprol resistance upon overexpression in culture. These findings offer new insights into Trypanosomatid basic biology, implications for drugs targets, and direct or indirect drug resistance mechanisms. This study generated a T. brucei ORFeome and Gain-of-Function parasite library, demonstrated the libraries’ usefulness in forward genetic screening, and identified novel aspects of melarsoprol resistance that will be the subject of future investigations. These powerful genetic tools can be used to broadly advance Trypanosomatid research.IMPORTANCETrypanosomatid parasites threaten the health of over 1 billion people worldwide. Because their genomes are highly diverged from well-established eukaryotes, conservation is not always useful in assigning gene functions. However, it is precisely among the Trypanosomatid-specific genes that ideal therapeutic targets might be found. Forward genetics approaches are an effective way to identify novel gene functions. We used an ORFeome approach to clone a large percentage of Trypanosoma brucei genes and generate a Gain-of-Function parasite library. This library was used in a genetic screen to identify genes that promote resistance to the clinically significant, yet highly toxic drug, melarsoprol. Hits arising from the screen demonstrated the library’s usefulness in identifying known pathways and uncovered novel aspects of resistance mediated by proteins localized to the flagellum and mitochondrion. The powerful new genetic tools generated herein are expected to promote advances in Trypanosomatid biology and therapeutic development in the years to come.

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Gamma-glutamylcysteine synthetase and tryparedoxin 1 exert high control on the antioxidant system in Trypanosoma cruzi contributing to drug resistance and infectivity

Cited by 24 publications

References 60 publications

Motility patterns of Trypanosoma cruzi trypomastigotes correlate with the efficiency of parasite invasion in vitro

Motility patterns of Trypanosoma cruzi trypomastigotes correlate with the efficiency of parasite invasion in vitro

Computational Drug Repositioning for Chagas Disease Using Protein-Ligand Interaction Profiling

ATrypanosoma bruceiORFeome-based Gain-of-Function Library identifies genes that promote survival during melarsoprol treatment

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