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Local and Systemic STAT3 and p65 NF-KappaB Expression as Progression Markers and Functional Targets for Patients With Cervical Cancer

Cervical cancer, which main etiologic factor is Human Papillomavirus (HPV) infection, continues to be a burden for public health systems in developing countries. Our laboratory has been working with the hypothesis that signals generated in the tumor microenvironment can modulate local and systemic i...

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Autores principales: Rossetti, Renata A. M., da Silva-Junior, Ildefonso A., Rodríguez, Gretel R., Alvarez, Karla L. F., Stone, Simone C., Cipelli, Marcella, Silveira, Caio R. F., Beldi, Mariana Carmezim, Mota, Giana R., Margarido, Paulo F. R., Baracat, Edmund C., Uno, Miyuki, Villa, Luisa L., Carvalho, Jesus P., Yokochi, Kaori, Rosa, Maria Beatriz S. F., Lorenzi, Noely P., Lepique, Ana Paula
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7710991/
https://www.ncbi.nlm.nih.gov/pubmed/33330068
http://dx.doi.org/10.3389/fonc.2020.587132
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author Rossetti, Renata A. M.
da Silva-Junior, Ildefonso A.
Rodríguez, Gretel R.
Alvarez, Karla L. F.
Stone, Simone C.
Cipelli, Marcella
Silveira, Caio R. F.
Beldi, Mariana Carmezim
Mota, Giana R.
Margarido, Paulo F. R.
Baracat, Edmund C.
Uno, Miyuki
Villa, Luisa L.
Carvalho, Jesus P.
Yokochi, Kaori
Rosa, Maria Beatriz S. F.
Lorenzi, Noely P.
Lepique, Ana Paula
author_facet Rossetti, Renata A. M.
da Silva-Junior, Ildefonso A.
Rodríguez, Gretel R.
Alvarez, Karla L. F.
Stone, Simone C.
Cipelli, Marcella
Silveira, Caio R. F.
Beldi, Mariana Carmezim
Mota, Giana R.
Margarido, Paulo F. R.
Baracat, Edmund C.
Uno, Miyuki
Villa, Luisa L.
Carvalho, Jesus P.
Yokochi, Kaori
Rosa, Maria Beatriz S. F.
Lorenzi, Noely P.
Lepique, Ana Paula
author_sort Rossetti, Renata A. M.
collection PubMed
description Cervical cancer, which main etiologic factor is Human Papillomavirus (HPV) infection, continues to be a burden for public health systems in developing countries. Our laboratory has been working with the hypothesis that signals generated in the tumor microenvironment can modulate local and systemic immune responses. In this context, it would be reasonable to think that tumors create pro-tumoral bias in immune cells, even before they are recruited to the tumor microenvironment. To understand if and how signaling started in the tumor microenvironment can influence cells within the tumor and systemically, we investigated the expression of key proteins in signaling pathways important for cell proliferation, viability, immune responses and tolerance. Besides, we used detection of specific phosphorylated residues, which are indicative of activation for Akt, CREB, p65 NFκB, and STAT3. Our findings included the observation of a significant STAT3 expression increase and p65 NFκB decrease in circulating leukocytes in correlation with lesion grade. In light of those observations, we started investigating the result of the inhibition of STAT3 in a tumor experimental model. STAT3 inhibition impaired tumor growth, increased anti-tumor T cell responses and decreased the accumulation of myeloid cells in the spleen. The concomitant inhibition of NFκB partially reversed these effects. This study indicates that STAT3 and NFκB are involved in immunomodulatory tumor effects and STAT3 inhibition could be considered as therapy for patients with cervical cancer.
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spelling pubmed-77109912020-12-15 Local and Systemic STAT3 and p65 NF-KappaB Expression as Progression Markers and Functional Targets for Patients With Cervical Cancer Rossetti, Renata A. M. da Silva-Junior, Ildefonso A. Rodríguez, Gretel R. Alvarez, Karla L. F. Stone, Simone C. Cipelli, Marcella Silveira, Caio R. F. Beldi, Mariana Carmezim Mota, Giana R. Margarido, Paulo F. R. Baracat, Edmund C. Uno, Miyuki Villa, Luisa L. Carvalho, Jesus P. Yokochi, Kaori Rosa, Maria Beatriz S. F. Lorenzi, Noely P. Lepique, Ana Paula Front Oncol Oncology Cervical cancer, which main etiologic factor is Human Papillomavirus (HPV) infection, continues to be a burden for public health systems in developing countries. Our laboratory has been working with the hypothesis that signals generated in the tumor microenvironment can modulate local and systemic immune responses. In this context, it would be reasonable to think that tumors create pro-tumoral bias in immune cells, even before they are recruited to the tumor microenvironment. To understand if and how signaling started in the tumor microenvironment can influence cells within the tumor and systemically, we investigated the expression of key proteins in signaling pathways important for cell proliferation, viability, immune responses and tolerance. Besides, we used detection of specific phosphorylated residues, which are indicative of activation for Akt, CREB, p65 NFκB, and STAT3. Our findings included the observation of a significant STAT3 expression increase and p65 NFκB decrease in circulating leukocytes in correlation with lesion grade. In light of those observations, we started investigating the result of the inhibition of STAT3 in a tumor experimental model. STAT3 inhibition impaired tumor growth, increased anti-tumor T cell responses and decreased the accumulation of myeloid cells in the spleen. The concomitant inhibition of NFκB partially reversed these effects. This study indicates that STAT3 and NFκB are involved in immunomodulatory tumor effects and STAT3 inhibition could be considered as therapy for patients with cervical cancer. Frontiers Media S.A. 2020-11-19 /pmc/articles/PMC7710991/ /pubmed/33330068 http://dx.doi.org/10.3389/fonc.2020.587132 Text en Copyright © 2020 Rossetti, da Silva-Junior, Rodríguez, Alvarez, Stone, Cipelli, Silveira, Beldi, Mota, Margarido, Baracat, Uno, Villa, Carvalho, Yokochi, Rosa, Lorenzi and Lepique http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Oncology
Rossetti, Renata A. M.
da Silva-Junior, Ildefonso A.
Rodríguez, Gretel R.
Alvarez, Karla L. F.
Stone, Simone C.
Cipelli, Marcella
Silveira, Caio R. F.
Beldi, Mariana Carmezim
Mota, Giana R.
Margarido, Paulo F. R.
Baracat, Edmund C.
Uno, Miyuki
Villa, Luisa L.
Carvalho, Jesus P.
Yokochi, Kaori
Rosa, Maria Beatriz S. F.
Lorenzi, Noely P.
Lepique, Ana Paula
Local and Systemic STAT3 and p65 NF-KappaB Expression as Progression Markers and Functional Targets for Patients With Cervical Cancer
title Local and Systemic STAT3 and p65 NF-KappaB Expression as Progression Markers and Functional Targets for Patients With Cervical Cancer
title_full Local and Systemic STAT3 and p65 NF-KappaB Expression as Progression Markers and Functional Targets for Patients With Cervical Cancer
title_fullStr Local and Systemic STAT3 and p65 NF-KappaB Expression as Progression Markers and Functional Targets for Patients With Cervical Cancer
title_full_unstemmed Local and Systemic STAT3 and p65 NF-KappaB Expression as Progression Markers and Functional Targets for Patients With Cervical Cancer
title_short Local and Systemic STAT3 and p65 NF-KappaB Expression as Progression Markers and Functional Targets for Patients With Cervical Cancer
title_sort local and systemic stat3 and p65 nf-kappab expression as progression markers and functional targets for patients with cervical cancer
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7710991/
https://www.ncbi.nlm.nih.gov/pubmed/33330068
http://dx.doi.org/10.3389/fonc.2020.587132
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