INPP4B is upregulated and functions as an oncogenic driver through SGK3 in a subset of melanomas

Inositol polyphosphate 4-phosphatase type II (INPP4B) negatively regulates PI3K/Akt signalling and has a tumour suppressive role in some types of cancers. However, we have found that it is upregulated in a subset of melanomas. Here we report that INPP4B can function as an oncogenic driver through ac...

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Autores principales: Chi, Meng Na, Guo, Su Tang, Wilmott, James S., Guo, Xiang Yun, Yan, Xu Guang, Wang, Chun Yan, Liu, Xiao Ying, Jin, Lei, Tseng, Hsin-Yi, Liu, Tao, Croft, Amanda, Hondermarck, Hubert, Scolyer, Richard A., Jiang, Chen Chen, Zhang, Xu Dong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4741868/
https://www.ncbi.nlm.nih.gov/pubmed/26573229
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author Chi, Meng Na
Guo, Su Tang
Wilmott, James S.
Guo, Xiang Yun
Yan, Xu Guang
Wang, Chun Yan
Liu, Xiao Ying
Jin, Lei
Tseng, Hsin-Yi
Liu, Tao
Croft, Amanda
Hondermarck, Hubert
Scolyer, Richard A.
Jiang, Chen Chen
Zhang, Xu Dong
author_facet Chi, Meng Na
Guo, Su Tang
Wilmott, James S.
Guo, Xiang Yun
Yan, Xu Guang
Wang, Chun Yan
Liu, Xiao Ying
Jin, Lei
Tseng, Hsin-Yi
Liu, Tao
Croft, Amanda
Hondermarck, Hubert
Scolyer, Richard A.
Jiang, Chen Chen
Zhang, Xu Dong
author_sort Chi, Meng Na
collection PubMed
description Inositol polyphosphate 4-phosphatase type II (INPP4B) negatively regulates PI3K/Akt signalling and has a tumour suppressive role in some types of cancers. However, we have found that it is upregulated in a subset of melanomas. Here we report that INPP4B can function as an oncogenic driver through activation of serum- and glucocorticoid-regulated kinase 3 (SGK3) in melanoma. While INPP4B knockdown inhibited melanoma cell proliferation and retarded melanoma xenograft growth, overexpression of INPP4B enhanced melanoma cell and melanocyte proliferation and triggered anchorage-independent growth of melanocytes. Noticeably, INPP4B-mediated melanoma cell proliferation was not related to activation of Akt, but was mediated by SGK3. Upregulation of INPP4B in melanoma cells was associated with loss of miRNA (miR)-494 and/or miR-599 due to gene copy number reduction. Indeed, overexpression of miR-494 or miR-599 downregulated INPP4B, reduced SGK3 activation, and inhibited melanoma cell proliferation, whereas introduction of anti-miR-494 or anti-miR-599 upregulated INPP4B, enhanced SGK3 activation, and promoted melanoma cell proliferation. Collectively, these results identify upregulation of INPP4B as an oncogenic mechanism through activation of SGK3 in a subset of melanomas, with implications for targeting INPP4B and restoring miR-494 and miR-599 as novel approaches in the treatment of melanomas with high INPP4B expression.
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spelling pubmed-47418682016-03-23 INPP4B is upregulated and functions as an oncogenic driver through SGK3 in a subset of melanomas Chi, Meng Na Guo, Su Tang Wilmott, James S. Guo, Xiang Yun Yan, Xu Guang Wang, Chun Yan Liu, Xiao Ying Jin, Lei Tseng, Hsin-Yi Liu, Tao Croft, Amanda Hondermarck, Hubert Scolyer, Richard A. Jiang, Chen Chen Zhang, Xu Dong Oncotarget Research Paper Inositol polyphosphate 4-phosphatase type II (INPP4B) negatively regulates PI3K/Akt signalling and has a tumour suppressive role in some types of cancers. However, we have found that it is upregulated in a subset of melanomas. Here we report that INPP4B can function as an oncogenic driver through activation of serum- and glucocorticoid-regulated kinase 3 (SGK3) in melanoma. While INPP4B knockdown inhibited melanoma cell proliferation and retarded melanoma xenograft growth, overexpression of INPP4B enhanced melanoma cell and melanocyte proliferation and triggered anchorage-independent growth of melanocytes. Noticeably, INPP4B-mediated melanoma cell proliferation was not related to activation of Akt, but was mediated by SGK3. Upregulation of INPP4B in melanoma cells was associated with loss of miRNA (miR)-494 and/or miR-599 due to gene copy number reduction. Indeed, overexpression of miR-494 or miR-599 downregulated INPP4B, reduced SGK3 activation, and inhibited melanoma cell proliferation, whereas introduction of anti-miR-494 or anti-miR-599 upregulated INPP4B, enhanced SGK3 activation, and promoted melanoma cell proliferation. Collectively, these results identify upregulation of INPP4B as an oncogenic mechanism through activation of SGK3 in a subset of melanomas, with implications for targeting INPP4B and restoring miR-494 and miR-599 as novel approaches in the treatment of melanomas with high INPP4B expression. Impact Journals LLC 2015-11-09 /pmc/articles/PMC4741868/ /pubmed/26573229 Text en Copyright: © 2015 Chi et al. http://creativecommons.org/licenses/by/2.5/ 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 credited.
spellingShingle Research Paper
Chi, Meng Na
Guo, Su Tang
Wilmott, James S.
Guo, Xiang Yun
Yan, Xu Guang
Wang, Chun Yan
Liu, Xiao Ying
Jin, Lei
Tseng, Hsin-Yi
Liu, Tao
Croft, Amanda
Hondermarck, Hubert
Scolyer, Richard A.
Jiang, Chen Chen
Zhang, Xu Dong
INPP4B is upregulated and functions as an oncogenic driver through SGK3 in a subset of melanomas
title INPP4B is upregulated and functions as an oncogenic driver through SGK3 in a subset of melanomas
title_full INPP4B is upregulated and functions as an oncogenic driver through SGK3 in a subset of melanomas
title_fullStr INPP4B is upregulated and functions as an oncogenic driver through SGK3 in a subset of melanomas
title_full_unstemmed INPP4B is upregulated and functions as an oncogenic driver through SGK3 in a subset of melanomas
title_short INPP4B is upregulated and functions as an oncogenic driver through SGK3 in a subset of melanomas
title_sort inpp4b is upregulated and functions as an oncogenic driver through sgk3 in a subset of melanomas
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4741868/
https://www.ncbi.nlm.nih.gov/pubmed/26573229
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