Cooperation between Apoptotic and Viable Metacyclics Enhances the Pathogenesis of Leishmaniasis

Mimicking mammalian apoptotic cells by exposing phosphatidylserine (PS) is a strategy used by virus and parasitic protozoa to escape host protective inflammatory responses. With Leishmania amazonensis (La), apoptotic mimicry is a prerogative of the intramacrophagic amastigote form of the parasite an...

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Autores principales: Wanderley, João Luiz Mendes, Pinto da Silva, Lucia Helena, Deolindo, Poliana, Soong, Lynn, Borges, Valéria Matos, Prates, Deboraci Brito, de Souza, Ana Paula Almeida, Barral, Aldina, Balanco, José Mario de Freitas, do Nascimento, Michelle Tanny Cunha, Saraiva, Elvira Maria, Barcinski, Marcello André
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2684641/
https://www.ncbi.nlm.nih.gov/pubmed/19478944
http://dx.doi.org/10.1371/journal.pone.0005733
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author Wanderley, João Luiz Mendes
Pinto da Silva, Lucia Helena
Deolindo, Poliana
Soong, Lynn
Borges, Valéria Matos
Prates, Deboraci Brito
de Souza, Ana Paula Almeida
Barral, Aldina
Balanco, José Mario de Freitas
do Nascimento, Michelle Tanny Cunha
Saraiva, Elvira Maria
Barcinski, Marcello André
author_facet Wanderley, João Luiz Mendes
Pinto da Silva, Lucia Helena
Deolindo, Poliana
Soong, Lynn
Borges, Valéria Matos
Prates, Deboraci Brito
de Souza, Ana Paula Almeida
Barral, Aldina
Balanco, José Mario de Freitas
do Nascimento, Michelle Tanny Cunha
Saraiva, Elvira Maria
Barcinski, Marcello André
author_sort Wanderley, João Luiz Mendes
collection PubMed
description Mimicking mammalian apoptotic cells by exposing phosphatidylserine (PS) is a strategy used by virus and parasitic protozoa to escape host protective inflammatory responses. With Leishmania amazonensis (La), apoptotic mimicry is a prerogative of the intramacrophagic amastigote form of the parasite and is modulated by the host. Now we show that differently from what happens with amastigotes, promastigotes exposing PS are non-viable, non-infective cells, undergoing apoptotic death. As part of the normal metacyclogenic process occurring in axenic cultures and in the gut of sand fly vectors, a sub-population of metacyclic promastigotes exposes PS. Apoptotic death of the purified PS-positive (PS(POS)) sub-population was confirmed by TUNEL staining and DNA laddering. Transmission electron microscopy revealed morphological alterations in PS(POS) metacyclics such as DNA condensation, cytoplasm degradation and mitochondrion and kinetoplast destruction, both in in vitro cultures and in sand fly guts. TUNEL(POS) promastigotes were detected only in the anterior midgut to foregut boundary of infected sand flies. Interestingly, caspase inhibitors modulated parasite death and PS exposure, when added to parasite cultures in a specific time window. Efficient in vitro macrophage infections and in vivo lesions only occur when PS(POS) and PS-negative (PS(NEG)) parasites were simultaneously added to the cell culture or inoculated in the mammalian host. The viable PS(NEG) promastigote was the infective form, as shown by following the fate of fluorescently labeled parasites, while the PS(POS) apoptotic sub-population inhibited host macrophage inflammatory response. PS exposure and macrophage inhibition by a subpopulation of promastigotes is a different mechanism than the one previously described with amastigotes, where the entire population exposes PS. Both mechanisms co-exist and play a role in the transmission and development of the disease in case of infection by La. Since both processes confer selective advantages to the infective microorganism they justify the occurrence of apoptotic features in a unicellular pathogen.
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spelling pubmed-26846412009-05-29 Cooperation between Apoptotic and Viable Metacyclics Enhances the Pathogenesis of Leishmaniasis Wanderley, João Luiz Mendes Pinto da Silva, Lucia Helena Deolindo, Poliana Soong, Lynn Borges, Valéria Matos Prates, Deboraci Brito de Souza, Ana Paula Almeida Barral, Aldina Balanco, José Mario de Freitas do Nascimento, Michelle Tanny Cunha Saraiva, Elvira Maria Barcinski, Marcello André PLoS One Research Article Mimicking mammalian apoptotic cells by exposing phosphatidylserine (PS) is a strategy used by virus and parasitic protozoa to escape host protective inflammatory responses. With Leishmania amazonensis (La), apoptotic mimicry is a prerogative of the intramacrophagic amastigote form of the parasite and is modulated by the host. Now we show that differently from what happens with amastigotes, promastigotes exposing PS are non-viable, non-infective cells, undergoing apoptotic death. As part of the normal metacyclogenic process occurring in axenic cultures and in the gut of sand fly vectors, a sub-population of metacyclic promastigotes exposes PS. Apoptotic death of the purified PS-positive (PS(POS)) sub-population was confirmed by TUNEL staining and DNA laddering. Transmission electron microscopy revealed morphological alterations in PS(POS) metacyclics such as DNA condensation, cytoplasm degradation and mitochondrion and kinetoplast destruction, both in in vitro cultures and in sand fly guts. TUNEL(POS) promastigotes were detected only in the anterior midgut to foregut boundary of infected sand flies. Interestingly, caspase inhibitors modulated parasite death and PS exposure, when added to parasite cultures in a specific time window. Efficient in vitro macrophage infections and in vivo lesions only occur when PS(POS) and PS-negative (PS(NEG)) parasites were simultaneously added to the cell culture or inoculated in the mammalian host. The viable PS(NEG) promastigote was the infective form, as shown by following the fate of fluorescently labeled parasites, while the PS(POS) apoptotic sub-population inhibited host macrophage inflammatory response. PS exposure and macrophage inhibition by a subpopulation of promastigotes is a different mechanism than the one previously described with amastigotes, where the entire population exposes PS. Both mechanisms co-exist and play a role in the transmission and development of the disease in case of infection by La. Since both processes confer selective advantages to the infective microorganism they justify the occurrence of apoptotic features in a unicellular pathogen. Public Library of Science 2009-05-29 /pmc/articles/PMC2684641/ /pubmed/19478944 http://dx.doi.org/10.1371/journal.pone.0005733 Text en Wanderley 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
Wanderley, João Luiz Mendes
Pinto da Silva, Lucia Helena
Deolindo, Poliana
Soong, Lynn
Borges, Valéria Matos
Prates, Deboraci Brito
de Souza, Ana Paula Almeida
Barral, Aldina
Balanco, José Mario de Freitas
do Nascimento, Michelle Tanny Cunha
Saraiva, Elvira Maria
Barcinski, Marcello André
Cooperation between Apoptotic and Viable Metacyclics Enhances the Pathogenesis of Leishmaniasis
title Cooperation between Apoptotic and Viable Metacyclics Enhances the Pathogenesis of Leishmaniasis
title_full Cooperation between Apoptotic and Viable Metacyclics Enhances the Pathogenesis of Leishmaniasis
title_fullStr Cooperation between Apoptotic and Viable Metacyclics Enhances the Pathogenesis of Leishmaniasis
title_full_unstemmed Cooperation between Apoptotic and Viable Metacyclics Enhances the Pathogenesis of Leishmaniasis
title_short Cooperation between Apoptotic and Viable Metacyclics Enhances the Pathogenesis of Leishmaniasis
title_sort cooperation between apoptotic and viable metacyclics enhances the pathogenesis of leishmaniasis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2684641/
https://www.ncbi.nlm.nih.gov/pubmed/19478944
http://dx.doi.org/10.1371/journal.pone.0005733
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