Proliferation and Differentiation of Trypanosoma cruzi inside Its Vector Have a New Trigger: Redox Status

Trypanosoma cruzi proliferate and differentiate inside different compartments of triatomines gut that is the first environment encountered by T. cruzi. Due to its complex life cycle, the parasite is constantly exposed to reactive oxygen species (ROS). We tested the influence of the pro-oxidant molec...

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Autores principales: Nogueira, Natália P., Saraiva, Francis M. S., Sultano, Pedro E., Cunha, Paula R. B. B., Laranja, Gustavo A. T., Justo, Graça A., Sabino, Kátia C. C., Coelho, Marsen G. P., Rossini, Ana, Atella, Georgia C., Paes, Marcia C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4324650/
https://www.ncbi.nlm.nih.gov/pubmed/25671543
http://dx.doi.org/10.1371/journal.pone.0116712
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author Nogueira, Natália P.
Saraiva, Francis M. S.
Sultano, Pedro E.
Cunha, Paula R. B. B.
Laranja, Gustavo A. T.
Justo, Graça A.
Sabino, Kátia C. C.
Coelho, Marsen G. P.
Rossini, Ana
Atella, Georgia C.
Paes, Marcia C.
author_facet Nogueira, Natália P.
Saraiva, Francis M. S.
Sultano, Pedro E.
Cunha, Paula R. B. B.
Laranja, Gustavo A. T.
Justo, Graça A.
Sabino, Kátia C. C.
Coelho, Marsen G. P.
Rossini, Ana
Atella, Georgia C.
Paes, Marcia C.
author_sort Nogueira, Natália P.
collection PubMed
description Trypanosoma cruzi proliferate and differentiate inside different compartments of triatomines gut that is the first environment encountered by T. cruzi. Due to its complex life cycle, the parasite is constantly exposed to reactive oxygen species (ROS). We tested the influence of the pro-oxidant molecules H(2)O(2) and the superoxide generator, Paraquat, as well as, metabolism products of the vector, with distinct redox status, in the proliferation and metacyclogenesis. These molecules are heme, hemozoin and urate. We also tested the antioxidants NAC and GSH. Heme induced the proliferation of epimastigotes and impaired the metacyclogenesis. β-hematin, did not affect epimastigote proliferation but decreased parasite differentiation. Conversely, we show that urate, GSH and NAC dramatically impaired epimastigote proliferation and during metacyclogenesis, NAC and urate induced a significant increment of trypomastigotes and decreased the percentage of epimastigotes. We also quantified the parasite loads in the anterior and posterior midguts and in the rectum of the vector by qPCR. The treatment with the antioxidants increased the parasite loads in all midgut sections analyzed. In vivo, the group of vectors fed with reduced molecules showed an increment of trypomastigotes and decreased epimastigotes when analyzed by differential counting. Heme stimulated proliferation by increasing the cell number in the S and G2/M phases, whereas NAC arrested epimastigotes in G1 phase. NAC greatly increased the percentage of trypomastigotes. Taken together, these data show a shift in the triatomine gut microenvironment caused by the redox status may also influence T. cruzi biology inside the vector. In this scenario, oxidants act to turn on epimastigote proliferation while antioxidants seem to switch the cycle towards metacyclogenesis. This is a new insight that defines a key role for redox metabolism in governing the parasitic life cycle.
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spelling pubmed-43246502015-02-18 Proliferation and Differentiation of Trypanosoma cruzi inside Its Vector Have a New Trigger: Redox Status Nogueira, Natália P. Saraiva, Francis M. S. Sultano, Pedro E. Cunha, Paula R. B. B. Laranja, Gustavo A. T. Justo, Graça A. Sabino, Kátia C. C. Coelho, Marsen G. P. Rossini, Ana Atella, Georgia C. Paes, Marcia C. PLoS One Research Article Trypanosoma cruzi proliferate and differentiate inside different compartments of triatomines gut that is the first environment encountered by T. cruzi. Due to its complex life cycle, the parasite is constantly exposed to reactive oxygen species (ROS). We tested the influence of the pro-oxidant molecules H(2)O(2) and the superoxide generator, Paraquat, as well as, metabolism products of the vector, with distinct redox status, in the proliferation and metacyclogenesis. These molecules are heme, hemozoin and urate. We also tested the antioxidants NAC and GSH. Heme induced the proliferation of epimastigotes and impaired the metacyclogenesis. β-hematin, did not affect epimastigote proliferation but decreased parasite differentiation. Conversely, we show that urate, GSH and NAC dramatically impaired epimastigote proliferation and during metacyclogenesis, NAC and urate induced a significant increment of trypomastigotes and decreased the percentage of epimastigotes. We also quantified the parasite loads in the anterior and posterior midguts and in the rectum of the vector by qPCR. The treatment with the antioxidants increased the parasite loads in all midgut sections analyzed. In vivo, the group of vectors fed with reduced molecules showed an increment of trypomastigotes and decreased epimastigotes when analyzed by differential counting. Heme stimulated proliferation by increasing the cell number in the S and G2/M phases, whereas NAC arrested epimastigotes in G1 phase. NAC greatly increased the percentage of trypomastigotes. Taken together, these data show a shift in the triatomine gut microenvironment caused by the redox status may also influence T. cruzi biology inside the vector. In this scenario, oxidants act to turn on epimastigote proliferation while antioxidants seem to switch the cycle towards metacyclogenesis. This is a new insight that defines a key role for redox metabolism in governing the parasitic life cycle. Public Library of Science 2015-02-11 /pmc/articles/PMC4324650/ /pubmed/25671543 http://dx.doi.org/10.1371/journal.pone.0116712 Text en © 2015 Nogueira et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Nogueira, Natália P.
Saraiva, Francis M. S.
Sultano, Pedro E.
Cunha, Paula R. B. B.
Laranja, Gustavo A. T.
Justo, Graça A.
Sabino, Kátia C. C.
Coelho, Marsen G. P.
Rossini, Ana
Atella, Georgia C.
Paes, Marcia C.
Proliferation and Differentiation of Trypanosoma cruzi inside Its Vector Have a New Trigger: Redox Status
title Proliferation and Differentiation of Trypanosoma cruzi inside Its Vector Have a New Trigger: Redox Status
title_full Proliferation and Differentiation of Trypanosoma cruzi inside Its Vector Have a New Trigger: Redox Status
title_fullStr Proliferation and Differentiation of Trypanosoma cruzi inside Its Vector Have a New Trigger: Redox Status
title_full_unstemmed Proliferation and Differentiation of Trypanosoma cruzi inside Its Vector Have a New Trigger: Redox Status
title_short Proliferation and Differentiation of Trypanosoma cruzi inside Its Vector Have a New Trigger: Redox Status
title_sort proliferation and differentiation of trypanosoma cruzi inside its vector have a new trigger: redox status
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4324650/
https://www.ncbi.nlm.nih.gov/pubmed/25671543
http://dx.doi.org/10.1371/journal.pone.0116712
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