JRK is a positive regulator of Î²-catenin transcriptional activity commonly overexpressed in colon, breast and ovarian cancer

L. Pangon; I. Ng; M. Giry-Laterriere; N. Currey; A. Morgan; F. Benthani; P. N. Tran; S. Al-Sohaily; E. Segelov; B. L. Parker; M. J. Cowley; D.C. Wright; L. St Heaps; L. Carey; I. Rooman; M. R. J. Kohonen-Corish

doi:10.1038/onc.2015.347

JRK is a positive regulator of Î²-catenin transcriptional activity commonly overexpressed in colon, breast and ovarian cancer

L. Pangon, I. Ng, M. Giry-Laterriere, N. Currey, A. Morgan, F. Benthani, P. N. Tran, S. Al-Sohaily, E. Segelov, B. L. Parker, M. J. Cowley, D.C. Wright, L. St Heaps, L. Carey, I. Rooman, M. R. J. Kohonen-Corish

Western Sydney University

Research output: Contribution to journal › Article › peer-review

19 Citations (Scopus)

Abstract

The loss of Î²-catenin inhibitory components is a well-established mechanism of carcinogenesis but Î²-catenin hyperactivity can also be enhanced through its coactivators. Here we first interrogated a highly validated genomic screen and the largest repository of cancer genomics data and identified JRK as a potential new oncogene and therapeutic target of the Î²-catenin pathway. We proceeded to validate the oncogenic role of JRK in colon cancer cells and primary tumors. Consistent with a Î²-catenin activator function, depletion of JRK in several cancer cell lines repressed Î²-catenin transcriptional activity and reduced cell proliferation. Importantly, JRK expression was aberrantly elevated in 21% of colorectal cancers, 15% of breast and ovarian cancers and was associated with increased expression of Î²-catenin target genes and increased cell proliferation. This study shows that JRK is required for Î²-catenin hyperactivity regardless of the adenomatous polyposis coli/Î²-catenin mutation status and targeting JRK presents new opportunities for therapeutic intervention in cancer.

Original language	English
Pages (from-to)	2834-2841
Number of pages	8
Journal	Oncogene
Volume	35
Issue number	22
DOIs	https://doi.org/10.1038/onc.2015.347
Publication status	Published - 2016

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Pangon, L., Ng, I., Giry-Laterriere, M., Currey, N., Morgan, A., Benthani, F., Tran, P. N., Al-Sohaily, S., Segelov, E., Parker, B. L., Cowley, M. J., Wright, D. C., St Heaps, L., Carey, L., Rooman, I., & Kohonen-Corish, M. R. J. (2016). JRK is a positive regulator of Î²-catenin transcriptional activity commonly overexpressed in colon, breast and ovarian cancer. Oncogene, 35(22), 2834-2841. https://doi.org/10.1038/onc.2015.347

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title = "JRK is a positive regulator of {\^I}²-catenin transcriptional activity commonly overexpressed in colon, breast and ovarian cancer",

abstract = "The loss of {\^I}²-catenin inhibitory components is a well-established mechanism of carcinogenesis but {\^I}²-catenin hyperactivity can also be enhanced through its coactivators. Here we first interrogated a highly validated genomic screen and the largest repository of cancer genomics data and identified JRK as a potential new oncogene and therapeutic target of the {\^I}²-catenin pathway. We proceeded to validate the oncogenic role of JRK in colon cancer cells and primary tumors. Consistent with a {\^I}²-catenin activator function, depletion of JRK in several cancer cell lines repressed {\^I}²-catenin transcriptional activity and reduced cell proliferation. Importantly, JRK expression was aberrantly elevated in 21% of colorectal cancers, 15% of breast and ovarian cancers and was associated with increased expression of {\^I}²-catenin target genes and increased cell proliferation. This study shows that JRK is required for {\^I}²-catenin hyperactivity regardless of the adenomatous polyposis coli/{\^I}²-catenin mutation status and targeting JRK presents new opportunities for therapeutic intervention in cancer.",

author = "L. Pangon and I. Ng and M. Giry-Laterriere and N. Currey and A. Morgan and F. Benthani and Tran, {P. N.} and S. Al-Sohaily and E. Segelov and Parker, {B. L.} and Cowley, {M. J.} and D.C. Wright and {St Heaps}, L. and L. Carey and I. Rooman and Kohonen-Corish, {M. R. J.}",

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Pangon, L, Ng, I, Giry-Laterriere, M, Currey, N, Morgan, A, Benthani, F, Tran, PN, Al-Sohaily, S, Segelov, E, Parker, BL, Cowley, MJ, Wright, DC, St Heaps, L, Carey, L, Rooman, I & Kohonen-Corish, MRJ 2016, 'JRK is a positive regulator of Î²-catenin transcriptional activity commonly overexpressed in colon, breast and ovarian cancer', Oncogene, vol. 35, no. 22, pp. 2834-2841. https://doi.org/10.1038/onc.2015.347

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T1 - JRK is a positive regulator of Î²-catenin transcriptional activity commonly overexpressed in colon, breast and ovarian cancer

AU - Pangon, L.

AU - Ng, I.

AU - Giry-Laterriere, M.

AU - Currey, N.

AU - Morgan, A.

AU - Benthani, F.

AU - Tran, P. N.

AU - Al-Sohaily, S.

AU - Segelov, E.

AU - Parker, B. L.

AU - Cowley, M. J.

AU - Wright, D.C.

AU - St Heaps, L.

AU - Carey, L.

AU - Rooman, I.

AU - Kohonen-Corish, M. R. J.

PY - 2016

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N2 - The loss of Î²-catenin inhibitory components is a well-established mechanism of carcinogenesis but Î²-catenin hyperactivity can also be enhanced through its coactivators. Here we first interrogated a highly validated genomic screen and the largest repository of cancer genomics data and identified JRK as a potential new oncogene and therapeutic target of the Î²-catenin pathway. We proceeded to validate the oncogenic role of JRK in colon cancer cells and primary tumors. Consistent with a Î²-catenin activator function, depletion of JRK in several cancer cell lines repressed Î²-catenin transcriptional activity and reduced cell proliferation. Importantly, JRK expression was aberrantly elevated in 21% of colorectal cancers, 15% of breast and ovarian cancers and was associated with increased expression of Î²-catenin target genes and increased cell proliferation. This study shows that JRK is required for Î²-catenin hyperactivity regardless of the adenomatous polyposis coli/Î²-catenin mutation status and targeting JRK presents new opportunities for therapeutic intervention in cancer.

AB - The loss of Î²-catenin inhibitory components is a well-established mechanism of carcinogenesis but Î²-catenin hyperactivity can also be enhanced through its coactivators. Here we first interrogated a highly validated genomic screen and the largest repository of cancer genomics data and identified JRK as a potential new oncogene and therapeutic target of the Î²-catenin pathway. We proceeded to validate the oncogenic role of JRK in colon cancer cells and primary tumors. Consistent with a Î²-catenin activator function, depletion of JRK in several cancer cell lines repressed Î²-catenin transcriptional activity and reduced cell proliferation. Importantly, JRK expression was aberrantly elevated in 21% of colorectal cancers, 15% of breast and ovarian cancers and was associated with increased expression of Î²-catenin target genes and increased cell proliferation. This study shows that JRK is required for Î²-catenin hyperactivity regardless of the adenomatous polyposis coli/Î²-catenin mutation status and targeting JRK presents new opportunities for therapeutic intervention in cancer.

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JRK is a positive regulator of Î²-catenin transcriptional activity commonly overexpressed in colon, breast and ovarian cancer

Abstract

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