Critical role of SIK3 in mediating high salt and IL-17 synergy leading to breast cancer cell proliferation

Chronic inflammation is a well-known precursor for cancer development and proliferation. We have recently demonstrated that high salt (NaCl) synergizes with sub-effective interleukin (IL)-17 to induce breast cancer cell proliferation. However, the exact molecular mechanisms mediating this effect are...

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Autores principales: Amara, Suneetha, Majors, Ciera, Roy, Bipradas, Hill, Salisha, Rose, Kristie L., Myles, Elbert L., Tiriveedhi, Venkataswarup
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5489190/
https://www.ncbi.nlm.nih.gov/pubmed/28658303
http://dx.doi.org/10.1371/journal.pone.0180097
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author Amara, Suneetha
Majors, Ciera
Roy, Bipradas
Hill, Salisha
Rose, Kristie L.
Myles, Elbert L.
Tiriveedhi, Venkataswarup
author_facet Amara, Suneetha
Majors, Ciera
Roy, Bipradas
Hill, Salisha
Rose, Kristie L.
Myles, Elbert L.
Tiriveedhi, Venkataswarup
author_sort Amara, Suneetha
collection PubMed
description Chronic inflammation is a well-known precursor for cancer development and proliferation. We have recently demonstrated that high salt (NaCl) synergizes with sub-effective interleukin (IL)-17 to induce breast cancer cell proliferation. However, the exact molecular mechanisms mediating this effect are unclear. In our current study, we adopted a phosphoproteomic-based approach to identify salt modulated kinase-proteome specific molecular targets. The phosphoprotemics based binary comparison between heavy labelled MCF-7 cells treated with high salt (Δ0.05 M NaCl) and light labelled MCF-7 cells cultured under basal conditions demonstrated an enhanced phosphorylation of Serine-493 of SIK3 protein. The mRNA transcript and protein expression analysis of SIK3 in MCF-7 cells demonstrated a synergistic enhancement following co-treatment with high salt and sub-effective IL-17 (0.1 ng/mL), as compared to either treatments alone. A similar increase in SIK3 expression was observed in other breast cancer cell lines, MDA-MB-231, BT20, and AU565, while non-malignant breast epithelial cell line, MCF10A, did not induce SIK3 expression under similar conditions. Biochemical studies revealed mTORC2 acted as upstream mediator of SIK3 phosphorylation. Importantly, cell cycle analysis by flow cytometry demonstrated SIK3 induced G0/G1-phase release mediated cell proliferation, while SIK3 silencing abolished this effect. Also, SIK3 induced pro-inflammatory arginine metabolism, as evidenced by upregulation of the enzymes iNOS and ASS-1, along with downregulation of anti-inflammatory enzymes, arginase-1 and ornithine decarboxylase. Furthermore, gelatin zymography analysis has demonstrated that SIK3 induced expression of tumor metastatic CXCR4 through MMP-9 activation. Taken together, our data suggests a critical role of SIK3 in mediating three important hallmarks of cancer namely, cell proliferation, inflammation and metastasis. These studies provide a mechanistic basis for the future utilization of SIK3 as a key drug discovery target to improve breast cancer therapy.
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spelling pubmed-54891902017-07-11 Critical role of SIK3 in mediating high salt and IL-17 synergy leading to breast cancer cell proliferation Amara, Suneetha Majors, Ciera Roy, Bipradas Hill, Salisha Rose, Kristie L. Myles, Elbert L. Tiriveedhi, Venkataswarup PLoS One Research Article Chronic inflammation is a well-known precursor for cancer development and proliferation. We have recently demonstrated that high salt (NaCl) synergizes with sub-effective interleukin (IL)-17 to induce breast cancer cell proliferation. However, the exact molecular mechanisms mediating this effect are unclear. In our current study, we adopted a phosphoproteomic-based approach to identify salt modulated kinase-proteome specific molecular targets. The phosphoprotemics based binary comparison between heavy labelled MCF-7 cells treated with high salt (Δ0.05 M NaCl) and light labelled MCF-7 cells cultured under basal conditions demonstrated an enhanced phosphorylation of Serine-493 of SIK3 protein. The mRNA transcript and protein expression analysis of SIK3 in MCF-7 cells demonstrated a synergistic enhancement following co-treatment with high salt and sub-effective IL-17 (0.1 ng/mL), as compared to either treatments alone. A similar increase in SIK3 expression was observed in other breast cancer cell lines, MDA-MB-231, BT20, and AU565, while non-malignant breast epithelial cell line, MCF10A, did not induce SIK3 expression under similar conditions. Biochemical studies revealed mTORC2 acted as upstream mediator of SIK3 phosphorylation. Importantly, cell cycle analysis by flow cytometry demonstrated SIK3 induced G0/G1-phase release mediated cell proliferation, while SIK3 silencing abolished this effect. Also, SIK3 induced pro-inflammatory arginine metabolism, as evidenced by upregulation of the enzymes iNOS and ASS-1, along with downregulation of anti-inflammatory enzymes, arginase-1 and ornithine decarboxylase. Furthermore, gelatin zymography analysis has demonstrated that SIK3 induced expression of tumor metastatic CXCR4 through MMP-9 activation. Taken together, our data suggests a critical role of SIK3 in mediating three important hallmarks of cancer namely, cell proliferation, inflammation and metastasis. These studies provide a mechanistic basis for the future utilization of SIK3 as a key drug discovery target to improve breast cancer therapy. Public Library of Science 2017-06-28 /pmc/articles/PMC5489190/ /pubmed/28658303 http://dx.doi.org/10.1371/journal.pone.0180097 Text en © 2017 Amara 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Amara, Suneetha
Majors, Ciera
Roy, Bipradas
Hill, Salisha
Rose, Kristie L.
Myles, Elbert L.
Tiriveedhi, Venkataswarup
Critical role of SIK3 in mediating high salt and IL-17 synergy leading to breast cancer cell proliferation
title Critical role of SIK3 in mediating high salt and IL-17 synergy leading to breast cancer cell proliferation
title_full Critical role of SIK3 in mediating high salt and IL-17 synergy leading to breast cancer cell proliferation
title_fullStr Critical role of SIK3 in mediating high salt and IL-17 synergy leading to breast cancer cell proliferation
title_full_unstemmed Critical role of SIK3 in mediating high salt and IL-17 synergy leading to breast cancer cell proliferation
title_short Critical role of SIK3 in mediating high salt and IL-17 synergy leading to breast cancer cell proliferation
title_sort critical role of sik3 in mediating high salt and il-17 synergy leading to breast cancer cell proliferation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5489190/
https://www.ncbi.nlm.nih.gov/pubmed/28658303
http://dx.doi.org/10.1371/journal.pone.0180097
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