Human Survivin and Trypanosoma cruzi Calreticulin Act in Synergy against a Murine Melanoma In Vivo

Immune-based anti-tumor or anti-angiogenic therapies hold considerable promise for the treatment of cancer. The first approach seeks to activate tumor antigen-specific T lymphocytes while, the second, delays tumor growth by interfering with blood supply. Tumor Associated Antigens are often employed...

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Autores principales: Aguilar-Guzmán, Lorena, Lobos-González, Lorena, Rosas, Carlos, Vallejos, Gerardo, Falcón, Cristián, Sosoniuk, Eduardo, Coddou, Francisca, Leyton, Lisette, Lemus, David, Quest, Andrew F. G., Ferreira, Arturo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3995754/
https://www.ncbi.nlm.nih.gov/pubmed/24755644
http://dx.doi.org/10.1371/journal.pone.0095457
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author Aguilar-Guzmán, Lorena
Lobos-González, Lorena
Rosas, Carlos
Vallejos, Gerardo
Falcón, Cristián
Sosoniuk, Eduardo
Coddou, Francisca
Leyton, Lisette
Lemus, David
Quest, Andrew F. G.
Ferreira, Arturo
author_facet Aguilar-Guzmán, Lorena
Lobos-González, Lorena
Rosas, Carlos
Vallejos, Gerardo
Falcón, Cristián
Sosoniuk, Eduardo
Coddou, Francisca
Leyton, Lisette
Lemus, David
Quest, Andrew F. G.
Ferreira, Arturo
author_sort Aguilar-Guzmán, Lorena
collection PubMed
description Immune-based anti-tumor or anti-angiogenic therapies hold considerable promise for the treatment of cancer. The first approach seeks to activate tumor antigen-specific T lymphocytes while, the second, delays tumor growth by interfering with blood supply. Tumor Associated Antigens are often employed to target tumors with therapeutic drugs, but some are also essential for tumor viability. Survivin (Surv) is a member of the inhibitor of apoptosis protein family that is considered a Tumor Associated Antigen important for cancer cell viability and proliferation. On the other hand, Trypanosoma cruzi (the agent of Chagas’ disease) calreticulin (TcCRT) displays remarkable anti-angiogenic properties. Because these molecules are associated with different tumor targets, we reasoned that immunization with a Surv-encoding plasmid (pSurv) and concomitant TcCRT administration should generate a stronger anti-tumor response than application of either treatment separately. To evaluate this possibility, C57BL/6 mice were immunized with pSurv and challenged with an isogenic melanoma cell line that had been pre-incubated with recombinant TcCRT (rTcCRT). Following tumor cell inoculation, mice were injected with additional doses of rTcCRT. For the combined regimen we observed in mice that: i). Tumor growth was impaired, ii). Humoral anti-rTcCRT immunity was induced and, iii). In vitro rTcCRT bound to melanocytes, thereby promoting the incorporation of human C1q and subsequent macrophage phagocytosis of tumor cells. These observations are interpreted to reflect the consequence of the following sequence of events: rTcCRT anti-angiogenic activity leads to stress in tumor cells. Murine CRT is then translocated to the external membrane where, together with rTcCRT, complement C1 is captured, thus promoting tumor phagocytosis. Presentation of the Tumor Associated Antigen Surv induces the adaptive anti-tumor immunity and, independently, mediates anti-endothelial cell immunity leading to an important delay in tumor growth.
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spelling pubmed-39957542014-04-25 Human Survivin and Trypanosoma cruzi Calreticulin Act in Synergy against a Murine Melanoma In Vivo Aguilar-Guzmán, Lorena Lobos-González, Lorena Rosas, Carlos Vallejos, Gerardo Falcón, Cristián Sosoniuk, Eduardo Coddou, Francisca Leyton, Lisette Lemus, David Quest, Andrew F. G. Ferreira, Arturo PLoS One Research Article Immune-based anti-tumor or anti-angiogenic therapies hold considerable promise for the treatment of cancer. The first approach seeks to activate tumor antigen-specific T lymphocytes while, the second, delays tumor growth by interfering with blood supply. Tumor Associated Antigens are often employed to target tumors with therapeutic drugs, but some are also essential for tumor viability. Survivin (Surv) is a member of the inhibitor of apoptosis protein family that is considered a Tumor Associated Antigen important for cancer cell viability and proliferation. On the other hand, Trypanosoma cruzi (the agent of Chagas’ disease) calreticulin (TcCRT) displays remarkable anti-angiogenic properties. Because these molecules are associated with different tumor targets, we reasoned that immunization with a Surv-encoding plasmid (pSurv) and concomitant TcCRT administration should generate a stronger anti-tumor response than application of either treatment separately. To evaluate this possibility, C57BL/6 mice were immunized with pSurv and challenged with an isogenic melanoma cell line that had been pre-incubated with recombinant TcCRT (rTcCRT). Following tumor cell inoculation, mice were injected with additional doses of rTcCRT. For the combined regimen we observed in mice that: i). Tumor growth was impaired, ii). Humoral anti-rTcCRT immunity was induced and, iii). In vitro rTcCRT bound to melanocytes, thereby promoting the incorporation of human C1q and subsequent macrophage phagocytosis of tumor cells. These observations are interpreted to reflect the consequence of the following sequence of events: rTcCRT anti-angiogenic activity leads to stress in tumor cells. Murine CRT is then translocated to the external membrane where, together with rTcCRT, complement C1 is captured, thus promoting tumor phagocytosis. Presentation of the Tumor Associated Antigen Surv induces the adaptive anti-tumor immunity and, independently, mediates anti-endothelial cell immunity leading to an important delay in tumor growth. Public Library of Science 2014-04-22 /pmc/articles/PMC3995754/ /pubmed/24755644 http://dx.doi.org/10.1371/journal.pone.0095457 Text en © 2014 Aguilar-Guzman 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
Aguilar-Guzmán, Lorena
Lobos-González, Lorena
Rosas, Carlos
Vallejos, Gerardo
Falcón, Cristián
Sosoniuk, Eduardo
Coddou, Francisca
Leyton, Lisette
Lemus, David
Quest, Andrew F. G.
Ferreira, Arturo
Human Survivin and Trypanosoma cruzi Calreticulin Act in Synergy against a Murine Melanoma In Vivo
title Human Survivin and Trypanosoma cruzi Calreticulin Act in Synergy against a Murine Melanoma In Vivo
title_full Human Survivin and Trypanosoma cruzi Calreticulin Act in Synergy against a Murine Melanoma In Vivo
title_fullStr Human Survivin and Trypanosoma cruzi Calreticulin Act in Synergy against a Murine Melanoma In Vivo
title_full_unstemmed Human Survivin and Trypanosoma cruzi Calreticulin Act in Synergy against a Murine Melanoma In Vivo
title_short Human Survivin and Trypanosoma cruzi Calreticulin Act in Synergy against a Murine Melanoma In Vivo
title_sort human survivin and trypanosoma cruzi calreticulin act in synergy against a murine melanoma in vivo
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3995754/
https://www.ncbi.nlm.nih.gov/pubmed/24755644
http://dx.doi.org/10.1371/journal.pone.0095457
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