In Vitro Phenotypic, Genomic and Proteomic Characterization of a Cytokine-Resistant Murine β-TC3 Cell Line

Type 1 diabetes mellitus (T1DM) is caused by the selective destruction of insulin-producing β-cells. This process is mediated by cells of the immune system through release of nitric oxide, free radicals and pro-inflammatory cytokines, which induce a complex network of intracellular signalling cascad...

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Autores principales: Coppola, Antonina, Tomasello, Laura, Pizzolanti, Giuseppe, Pucci-Minafra, Ida, Albanese, Nadia, Di Cara, Gianluca, Cancemi, Patrizia, Pitrone, Maria, Bommarito, Alessandra, Carissimi, Elvira, Zito, Giovanni, Criscimanna, Angela, Galluzzo, Aldo, Giordano, Carla
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3290556/
https://www.ncbi.nlm.nih.gov/pubmed/22393382
http://dx.doi.org/10.1371/journal.pone.0032109
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author Coppola, Antonina
Tomasello, Laura
Pizzolanti, Giuseppe
Pucci-Minafra, Ida
Albanese, Nadia
Di Cara, Gianluca
Cancemi, Patrizia
Pitrone, Maria
Bommarito, Alessandra
Carissimi, Elvira
Zito, Giovanni
Criscimanna, Angela
Galluzzo, Aldo
Giordano, Carla
author_facet Coppola, Antonina
Tomasello, Laura
Pizzolanti, Giuseppe
Pucci-Minafra, Ida
Albanese, Nadia
Di Cara, Gianluca
Cancemi, Patrizia
Pitrone, Maria
Bommarito, Alessandra
Carissimi, Elvira
Zito, Giovanni
Criscimanna, Angela
Galluzzo, Aldo
Giordano, Carla
author_sort Coppola, Antonina
collection PubMed
description Type 1 diabetes mellitus (T1DM) is caused by the selective destruction of insulin-producing β-cells. This process is mediated by cells of the immune system through release of nitric oxide, free radicals and pro-inflammatory cytokines, which induce a complex network of intracellular signalling cascades, eventually affecting the expression of genes involved in β-cell survival. The aim of our study was to investigate possible mechanisms of resistance to cytokine-induced β-cell death. To this purpose, we created a cytokine-resistant β-cell line (β-TC3R) by chronically treating the β-TC3 murine insulinoma cell line with IL-1β + IFN-γ. β-TC3R cells exhibited higher proliferation rate and resistance to cytokine-mediated cell death in comparison to the parental line. Interestingly, they maintained expression of β-cell specific markers, such as PDX1, NKX6.1, GLUT2 and insulin. The analysis of the secretory function showed that β-TC3R cells have impaired glucose-induced c-peptide release, which however was only moderately reduced after incubation with KCl and tolbutamide. Gene expression analysis showed that β-TC3R cells were characterized by downregulation of IL-1β and IFN-γ receptors and upregulation of SOCS3, the classical negative regulator of cytokines signaling. Comparative proteomic analysis showed specific upregulation of 35 proteins, mainly involved in cell death, stress response and folding. Among them, SUMO4, a negative feedback regulator in NF-kB and JAK/STAT signaling pathways, resulted hyper-expressed. Silencing of SUMO4 was able to restore sensitivity to cytokine-induced cell death in β-TC3R cells, suggesting it may play a key role in acquired cytokine resistance by blocking JAK/STAT and NF-kB lethal signaling. In conclusion, our study represents the first extensive proteomic characterization of a murine cytokine-resistant β-cell line, which might represent a useful tool for studying the mechanisms involved in resistance to cytokine-mediated β-cell death. This knowledge may be of potential benefit for patients with T1DM. In particular, SUMO4 could be used as a therapeutical target.
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spelling pubmed-32905562012-03-05 In Vitro Phenotypic, Genomic and Proteomic Characterization of a Cytokine-Resistant Murine β-TC3 Cell Line Coppola, Antonina Tomasello, Laura Pizzolanti, Giuseppe Pucci-Minafra, Ida Albanese, Nadia Di Cara, Gianluca Cancemi, Patrizia Pitrone, Maria Bommarito, Alessandra Carissimi, Elvira Zito, Giovanni Criscimanna, Angela Galluzzo, Aldo Giordano, Carla PLoS One Research Article Type 1 diabetes mellitus (T1DM) is caused by the selective destruction of insulin-producing β-cells. This process is mediated by cells of the immune system through release of nitric oxide, free radicals and pro-inflammatory cytokines, which induce a complex network of intracellular signalling cascades, eventually affecting the expression of genes involved in β-cell survival. The aim of our study was to investigate possible mechanisms of resistance to cytokine-induced β-cell death. To this purpose, we created a cytokine-resistant β-cell line (β-TC3R) by chronically treating the β-TC3 murine insulinoma cell line with IL-1β + IFN-γ. β-TC3R cells exhibited higher proliferation rate and resistance to cytokine-mediated cell death in comparison to the parental line. Interestingly, they maintained expression of β-cell specific markers, such as PDX1, NKX6.1, GLUT2 and insulin. The analysis of the secretory function showed that β-TC3R cells have impaired glucose-induced c-peptide release, which however was only moderately reduced after incubation with KCl and tolbutamide. Gene expression analysis showed that β-TC3R cells were characterized by downregulation of IL-1β and IFN-γ receptors and upregulation of SOCS3, the classical negative regulator of cytokines signaling. Comparative proteomic analysis showed specific upregulation of 35 proteins, mainly involved in cell death, stress response and folding. Among them, SUMO4, a negative feedback regulator in NF-kB and JAK/STAT signaling pathways, resulted hyper-expressed. Silencing of SUMO4 was able to restore sensitivity to cytokine-induced cell death in β-TC3R cells, suggesting it may play a key role in acquired cytokine resistance by blocking JAK/STAT and NF-kB lethal signaling. In conclusion, our study represents the first extensive proteomic characterization of a murine cytokine-resistant β-cell line, which might represent a useful tool for studying the mechanisms involved in resistance to cytokine-mediated β-cell death. This knowledge may be of potential benefit for patients with T1DM. In particular, SUMO4 could be used as a therapeutical target. Public Library of Science 2012-02-29 /pmc/articles/PMC3290556/ /pubmed/22393382 http://dx.doi.org/10.1371/journal.pone.0032109 Text en Coppola 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
Coppola, Antonina
Tomasello, Laura
Pizzolanti, Giuseppe
Pucci-Minafra, Ida
Albanese, Nadia
Di Cara, Gianluca
Cancemi, Patrizia
Pitrone, Maria
Bommarito, Alessandra
Carissimi, Elvira
Zito, Giovanni
Criscimanna, Angela
Galluzzo, Aldo
Giordano, Carla
In Vitro Phenotypic, Genomic and Proteomic Characterization of a Cytokine-Resistant Murine β-TC3 Cell Line
title In Vitro Phenotypic, Genomic and Proteomic Characterization of a Cytokine-Resistant Murine β-TC3 Cell Line
title_full In Vitro Phenotypic, Genomic and Proteomic Characterization of a Cytokine-Resistant Murine β-TC3 Cell Line
title_fullStr In Vitro Phenotypic, Genomic and Proteomic Characterization of a Cytokine-Resistant Murine β-TC3 Cell Line
title_full_unstemmed In Vitro Phenotypic, Genomic and Proteomic Characterization of a Cytokine-Resistant Murine β-TC3 Cell Line
title_short In Vitro Phenotypic, Genomic and Proteomic Characterization of a Cytokine-Resistant Murine β-TC3 Cell Line
title_sort in vitro phenotypic, genomic and proteomic characterization of a cytokine-resistant murine β-tc3 cell line
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3290556/
https://www.ncbi.nlm.nih.gov/pubmed/22393382
http://dx.doi.org/10.1371/journal.pone.0032109
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