Molecular Mechanisms of Paraptosis Induction: Implications for a Non-Genetically Modified Tumor Vaccine

Paraptosis is the programmed cell death pathway that leads to cellular necrosis. Previously, rodent and human monocytes/macrophages killed glioma cells bearing the membrane macrophage colony stimulating factor (mM-CSF) through paraptosis, but the molecular mechanism of this killing process was never...

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Autores principales: Hoa, Neil, Myers, Michael P., Douglass, Thomas G., Zhang, Jian Gang, Delgado, Christina, Driggers, Lara, Callahan, Linda L., VanDeusen, Gerald, Pham, Jimmy T. H., Bhakta, Nirav, Ge, Lisheng, Jadus, Martin R.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2645013/
https://www.ncbi.nlm.nih.gov/pubmed/19247476
http://dx.doi.org/10.1371/journal.pone.0004631
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author Hoa, Neil
Myers, Michael P.
Douglass, Thomas G.
Zhang, Jian Gang
Delgado, Christina
Driggers, Lara
Callahan, Linda L.
VanDeusen, Gerald
Pham, Jimmy T. H.
Bhakta, Nirav
Ge, Lisheng
Jadus, Martin R.
author_facet Hoa, Neil
Myers, Michael P.
Douglass, Thomas G.
Zhang, Jian Gang
Delgado, Christina
Driggers, Lara
Callahan, Linda L.
VanDeusen, Gerald
Pham, Jimmy T. H.
Bhakta, Nirav
Ge, Lisheng
Jadus, Martin R.
author_sort Hoa, Neil
collection PubMed
description Paraptosis is the programmed cell death pathway that leads to cellular necrosis. Previously, rodent and human monocytes/macrophages killed glioma cells bearing the membrane macrophage colony stimulating factor (mM-CSF) through paraptosis, but the molecular mechanism of this killing process was never identified. We have demonstrated that paraptosis of rat T9 glioma cells can be initiated through a large potassium channel (BK)-dependent process initiated by reactive oxygen species. Macrophage mediated cytotoxicity upon the mM-CSF expressing T9-C2 cells was not prevented by the addition of the caspase inhibitor, zVAD-fmk. By a combination of fluorescent confocal and electron microscopy, flow cytometry, electrophysiology, pharmacology, and genetic knock-down approaches, we demonstrated that these ion channels control cellular swelling and vacuolization of rat T9 glioma cells. Cell lysis is preceded by a depletion of intracellular ATP. Six-hour exposure to BK channel activation caused T9 cells to over express heat shock proteins (Hsp 60, 70, 90 and gp96). This same treatment forced HMGB1 translocation from the nuclear region to the periphery. These last molecules are “danger signals” that can stimulate immune responses. Similar inductions of mitochondrial swelling and increased Hsp70 and 90 expressions by BK channel activation were observed with the non-immunogenic F98 glioma cells. Rats injected with T9 cells which were killed by prolonged BK channel activation developed immunity against the T9 cells, while the injection of x-irradiated apoptotic T9 cells failed to produce the vaccinating effect. These results are the first to show that glioma cellular death induced by prolonged BK channel activation improves tumor immunogenicity; this treatment reproduces the vaccinating effects of mM-CSF transduced cells. Elucidation of strategies as described in this study may prove quite valuable in the development of clinical immunotherapy against cancer.
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spelling pubmed-26450132009-02-27 Molecular Mechanisms of Paraptosis Induction: Implications for a Non-Genetically Modified Tumor Vaccine Hoa, Neil Myers, Michael P. Douglass, Thomas G. Zhang, Jian Gang Delgado, Christina Driggers, Lara Callahan, Linda L. VanDeusen, Gerald Pham, Jimmy T. H. Bhakta, Nirav Ge, Lisheng Jadus, Martin R. PLoS One Research Article Paraptosis is the programmed cell death pathway that leads to cellular necrosis. Previously, rodent and human monocytes/macrophages killed glioma cells bearing the membrane macrophage colony stimulating factor (mM-CSF) through paraptosis, but the molecular mechanism of this killing process was never identified. We have demonstrated that paraptosis of rat T9 glioma cells can be initiated through a large potassium channel (BK)-dependent process initiated by reactive oxygen species. Macrophage mediated cytotoxicity upon the mM-CSF expressing T9-C2 cells was not prevented by the addition of the caspase inhibitor, zVAD-fmk. By a combination of fluorescent confocal and electron microscopy, flow cytometry, electrophysiology, pharmacology, and genetic knock-down approaches, we demonstrated that these ion channels control cellular swelling and vacuolization of rat T9 glioma cells. Cell lysis is preceded by a depletion of intracellular ATP. Six-hour exposure to BK channel activation caused T9 cells to over express heat shock proteins (Hsp 60, 70, 90 and gp96). This same treatment forced HMGB1 translocation from the nuclear region to the periphery. These last molecules are “danger signals” that can stimulate immune responses. Similar inductions of mitochondrial swelling and increased Hsp70 and 90 expressions by BK channel activation were observed with the non-immunogenic F98 glioma cells. Rats injected with T9 cells which were killed by prolonged BK channel activation developed immunity against the T9 cells, while the injection of x-irradiated apoptotic T9 cells failed to produce the vaccinating effect. These results are the first to show that glioma cellular death induced by prolonged BK channel activation improves tumor immunogenicity; this treatment reproduces the vaccinating effects of mM-CSF transduced cells. Elucidation of strategies as described in this study may prove quite valuable in the development of clinical immunotherapy against cancer. Public Library of Science 2009-02-27 /pmc/articles/PMC2645013/ /pubmed/19247476 http://dx.doi.org/10.1371/journal.pone.0004631 Text en This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Hoa, Neil
Myers, Michael P.
Douglass, Thomas G.
Zhang, Jian Gang
Delgado, Christina
Driggers, Lara
Callahan, Linda L.
VanDeusen, Gerald
Pham, Jimmy T. H.
Bhakta, Nirav
Ge, Lisheng
Jadus, Martin R.
Molecular Mechanisms of Paraptosis Induction: Implications for a Non-Genetically Modified Tumor Vaccine
title Molecular Mechanisms of Paraptosis Induction: Implications for a Non-Genetically Modified Tumor Vaccine
title_full Molecular Mechanisms of Paraptosis Induction: Implications for a Non-Genetically Modified Tumor Vaccine
title_fullStr Molecular Mechanisms of Paraptosis Induction: Implications for a Non-Genetically Modified Tumor Vaccine
title_full_unstemmed Molecular Mechanisms of Paraptosis Induction: Implications for a Non-Genetically Modified Tumor Vaccine
title_short Molecular Mechanisms of Paraptosis Induction: Implications for a Non-Genetically Modified Tumor Vaccine
title_sort molecular mechanisms of paraptosis induction: implications for a non-genetically modified tumor vaccine
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2645013/
https://www.ncbi.nlm.nih.gov/pubmed/19247476
http://dx.doi.org/10.1371/journal.pone.0004631
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