Apigenin Increases SHIP-1 Expression, Promotes Tumoricidal Macrophages and Anti-Tumor Immune Responses in Murine Pancreatic Cancer

SIMPLE SUMMARY: Src Homology 2 (SH2) domain-containing Inositol 5’-Phosphatase-1 (SHIP-1) is an essential protein and the master regulator of myeloid cell development and function that impacts tumor immunity. We previously published that SHIP-1 regulates the expansion and function of immunosuppressi...

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Autores principales: Villalobos-Ayala, Krystal, Ortiz Rivera, Ivannie, Alvarez, Ciara, Husain, Kazim, DeLoach, DeVon, Krystal, Gerald, Hibbs, Margaret L., Jiang, Kun, Ghansah, Tomar
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7761852/
https://www.ncbi.nlm.nih.gov/pubmed/33291556
http://dx.doi.org/10.3390/cancers12123631
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author Villalobos-Ayala, Krystal
Ortiz Rivera, Ivannie
Alvarez, Ciara
Husain, Kazim
DeLoach, DeVon
Krystal, Gerald
Hibbs, Margaret L.
Jiang, Kun
Ghansah, Tomar
author_facet Villalobos-Ayala, Krystal
Ortiz Rivera, Ivannie
Alvarez, Ciara
Husain, Kazim
DeLoach, DeVon
Krystal, Gerald
Hibbs, Margaret L.
Jiang, Kun
Ghansah, Tomar
author_sort Villalobos-Ayala, Krystal
collection PubMed
description SIMPLE SUMMARY: Src Homology 2 (SH2) domain-containing Inositol 5’-Phosphatase-1 (SHIP-1) is an essential protein and the master regulator of myeloid cell development and function that impacts tumor immunity. We previously published that SHIP-1 regulates the expansion and function of immunosuppressive myeloid cells, which correlated with pancreatic cancer progression in mice. Here, we show that the bioflavonoid Apigenin restored SHIP-1 expression, significantly increased tumoricidal Tumor-Associated Macrophages (TAM) while significantly decreased immunosuppressive TAM percentages and improved anti-tumor immune responses in the tumor microenvironment using different pancreatic cancer models. Our research findings suggest that SHIP-1 may be a potential novel therapeutic target to promote the development of tumoricidal TAM that can assist in the treatment of pancreatic cancer. ABSTRACT: Pancreatic cancer (PC) has an extremely poor prognosis due to the expansion of immunosuppressive myeloid-derived suppressor cells (MDSC) and tumor-associated macrophages (TAM) in the inflammatory tumor microenvironment (TME), which halts the recruitment of effector immune cells and renders immunotherapy ineffective. Thus, the identification of new molecular targets that can modulate the immunosuppressive TME is warranted for PC intervention. Src Homology-2 (SH2) domain-containing Inositol 5′-Phosphatase-1 (SHIP-1) is a lipid signaling protein and a regulator of myeloid cell development and function. Herein, we used the bioflavonoid apigenin (API) to reduce inflammation in different PC models. Wild type mice harboring heterotopic or orthotopic PC were treated with API, which induced SHIP-1 expression, reduced inflammatory tumor-derived factors (TDF), increased the proportion of tumoricidal macrophages and enhanced anti-tumor immune responses, resulting in a reduction in tumor burden compared to vehicle-treated PC mice. In contrast, SHIP-1-deficient mice exhibited an increased tumor burden and displayed augmented proportions of pro-tumor macrophages. These results provide further support for the importance of SHIP-1 expression in promoting pro-tumor macrophage development in the pancreatic TME. Our findings suggest that agents augmenting SHIP-1 expression may provide novel therapeutic options for the treatment of PC.
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spelling pubmed-77618522020-12-26 Apigenin Increases SHIP-1 Expression, Promotes Tumoricidal Macrophages and Anti-Tumor Immune Responses in Murine Pancreatic Cancer Villalobos-Ayala, Krystal Ortiz Rivera, Ivannie Alvarez, Ciara Husain, Kazim DeLoach, DeVon Krystal, Gerald Hibbs, Margaret L. Jiang, Kun Ghansah, Tomar Cancers (Basel) Article SIMPLE SUMMARY: Src Homology 2 (SH2) domain-containing Inositol 5’-Phosphatase-1 (SHIP-1) is an essential protein and the master regulator of myeloid cell development and function that impacts tumor immunity. We previously published that SHIP-1 regulates the expansion and function of immunosuppressive myeloid cells, which correlated with pancreatic cancer progression in mice. Here, we show that the bioflavonoid Apigenin restored SHIP-1 expression, significantly increased tumoricidal Tumor-Associated Macrophages (TAM) while significantly decreased immunosuppressive TAM percentages and improved anti-tumor immune responses in the tumor microenvironment using different pancreatic cancer models. Our research findings suggest that SHIP-1 may be a potential novel therapeutic target to promote the development of tumoricidal TAM that can assist in the treatment of pancreatic cancer. ABSTRACT: Pancreatic cancer (PC) has an extremely poor prognosis due to the expansion of immunosuppressive myeloid-derived suppressor cells (MDSC) and tumor-associated macrophages (TAM) in the inflammatory tumor microenvironment (TME), which halts the recruitment of effector immune cells and renders immunotherapy ineffective. Thus, the identification of new molecular targets that can modulate the immunosuppressive TME is warranted for PC intervention. Src Homology-2 (SH2) domain-containing Inositol 5′-Phosphatase-1 (SHIP-1) is a lipid signaling protein and a regulator of myeloid cell development and function. Herein, we used the bioflavonoid apigenin (API) to reduce inflammation in different PC models. Wild type mice harboring heterotopic or orthotopic PC were treated with API, which induced SHIP-1 expression, reduced inflammatory tumor-derived factors (TDF), increased the proportion of tumoricidal macrophages and enhanced anti-tumor immune responses, resulting in a reduction in tumor burden compared to vehicle-treated PC mice. In contrast, SHIP-1-deficient mice exhibited an increased tumor burden and displayed augmented proportions of pro-tumor macrophages. These results provide further support for the importance of SHIP-1 expression in promoting pro-tumor macrophage development in the pancreatic TME. Our findings suggest that agents augmenting SHIP-1 expression may provide novel therapeutic options for the treatment of PC. MDPI 2020-12-04 /pmc/articles/PMC7761852/ /pubmed/33291556 http://dx.doi.org/10.3390/cancers12123631 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Villalobos-Ayala, Krystal
Ortiz Rivera, Ivannie
Alvarez, Ciara
Husain, Kazim
DeLoach, DeVon
Krystal, Gerald
Hibbs, Margaret L.
Jiang, Kun
Ghansah, Tomar
Apigenin Increases SHIP-1 Expression, Promotes Tumoricidal Macrophages and Anti-Tumor Immune Responses in Murine Pancreatic Cancer
title Apigenin Increases SHIP-1 Expression, Promotes Tumoricidal Macrophages and Anti-Tumor Immune Responses in Murine Pancreatic Cancer
title_full Apigenin Increases SHIP-1 Expression, Promotes Tumoricidal Macrophages and Anti-Tumor Immune Responses in Murine Pancreatic Cancer
title_fullStr Apigenin Increases SHIP-1 Expression, Promotes Tumoricidal Macrophages and Anti-Tumor Immune Responses in Murine Pancreatic Cancer
title_full_unstemmed Apigenin Increases SHIP-1 Expression, Promotes Tumoricidal Macrophages and Anti-Tumor Immune Responses in Murine Pancreatic Cancer
title_short Apigenin Increases SHIP-1 Expression, Promotes Tumoricidal Macrophages and Anti-Tumor Immune Responses in Murine Pancreatic Cancer
title_sort apigenin increases ship-1 expression, promotes tumoricidal macrophages and anti-tumor immune responses in murine pancreatic cancer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7761852/
https://www.ncbi.nlm.nih.gov/pubmed/33291556
http://dx.doi.org/10.3390/cancers12123631
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