SOX4 interacts with plakoglobin in a Wnt3a-dependent manner in prostate cancer cells

<p>Abstract</p> <p>Background</p> <p>SOX4 is a developmental transcription factor that is required for differentiation and proliferation in multiple tissues. SOX4 is overexpressed in many human malignancies, but the precise role of SOX4 in cancer progression is still no...

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Main Authors: Lai Yu-Heng, Cheng Jessica, Cheng Dongmei, Feasel Mattie E, Beste Kyle D, Peng Junmin, Nusrat Asma, Moreno Carlos S
Format: Article
Language:English
Published: BMC 2011-11-01
Series:BMC Cell Biology
Online Access:http://www.biomedcentral.com/1471-2121/12/50
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spelling doaj-a03980eb7e6b4317aa72c0b90e55858e2020-11-25T02:31:26ZengBMCBMC Cell Biology1471-21212011-11-011215010.1186/1471-2121-12-50SOX4 interacts with plakoglobin in a Wnt3a-dependent manner in prostate cancer cellsLai Yu-HengCheng JessicaCheng DongmeiFeasel Mattie EBeste Kyle DPeng JunminNusrat AsmaMoreno Carlos S<p>Abstract</p> <p>Background</p> <p>SOX4 is a developmental transcription factor that is required for differentiation and proliferation in multiple tissues. SOX4 is overexpressed in many human malignancies, but the precise role of SOX4 in cancer progression is still not well understood. Thus, the identification of additional SOX4 binding partners is essential for elucidating the mechanism of SOX4-mediated effects in cancer progression.</p> <p>Results</p> <p>Here, we have adapted a one-step affinity purification method that enables rapid purification of SOX4 complexes via intracellular biotinylation of the amino-terminus of SOX4 to perform large-scale proteomics analysis. We have discovered that junction plakoglobin (JUP) interacts with SOX4 in both the cytosol and the nucleus and the interaction between SOX4 and plakoglobin is significantly increased when prostate and breast cancer cells are stimulated with WNT3A. Interactions between SOX4 and plakoglobin were further enhanced by the nuclear export inhibitor leptomycin B (LMB), suggesting that plakoglobin promotes nuclear export of SOX4. The SOX4-plakoglobin complex affected the expression of Wnt pathway target genes and SOX4 downstream targets, such as <it>AXIN2</it>, <it>DICER1</it>, and <it>DHX9</it>. In addition, SOX4 DNA binding activity to the promoters of <it>DICER1</it>, <it>AXIN2</it>, <it>DHX9 </it>and <it>SOX4 </it>itself was reduced by conditions that promote SOX4-plakoglobin complex formation. Conditions that enhanced SOX4-plakoglobin interactions resulted in reduced transcriptional activity of β-catenin luciferase reporters.</p> <p>Conclusions</p> <p>These data suggest that this newly identified interaction between SOX4 and plakoglobin is inhibitory and provides new insights into the role of SOX4 in key pathways in cell proliferation, development, and cancer progression.</p> http://www.biomedcentral.com/1471-2121/12/50
collection DOAJ
language English
format Article
sources DOAJ
author Lai Yu-Heng
Cheng Jessica
Cheng Dongmei
Feasel Mattie E
Beste Kyle D
Peng Junmin
Nusrat Asma
Moreno Carlos S
spellingShingle Lai Yu-Heng
Cheng Jessica
Cheng Dongmei
Feasel Mattie E
Beste Kyle D
Peng Junmin
Nusrat Asma
Moreno Carlos S
SOX4 interacts with plakoglobin in a Wnt3a-dependent manner in prostate cancer cells
BMC Cell Biology
author_facet Lai Yu-Heng
Cheng Jessica
Cheng Dongmei
Feasel Mattie E
Beste Kyle D
Peng Junmin
Nusrat Asma
Moreno Carlos S
author_sort Lai Yu-Heng
title SOX4 interacts with plakoglobin in a Wnt3a-dependent manner in prostate cancer cells
title_short SOX4 interacts with plakoglobin in a Wnt3a-dependent manner in prostate cancer cells
title_full SOX4 interacts with plakoglobin in a Wnt3a-dependent manner in prostate cancer cells
title_fullStr SOX4 interacts with plakoglobin in a Wnt3a-dependent manner in prostate cancer cells
title_full_unstemmed SOX4 interacts with plakoglobin in a Wnt3a-dependent manner in prostate cancer cells
title_sort sox4 interacts with plakoglobin in a wnt3a-dependent manner in prostate cancer cells
publisher BMC
series BMC Cell Biology
issn 1471-2121
publishDate 2011-11-01
description <p>Abstract</p> <p>Background</p> <p>SOX4 is a developmental transcription factor that is required for differentiation and proliferation in multiple tissues. SOX4 is overexpressed in many human malignancies, but the precise role of SOX4 in cancer progression is still not well understood. Thus, the identification of additional SOX4 binding partners is essential for elucidating the mechanism of SOX4-mediated effects in cancer progression.</p> <p>Results</p> <p>Here, we have adapted a one-step affinity purification method that enables rapid purification of SOX4 complexes via intracellular biotinylation of the amino-terminus of SOX4 to perform large-scale proteomics analysis. We have discovered that junction plakoglobin (JUP) interacts with SOX4 in both the cytosol and the nucleus and the interaction between SOX4 and plakoglobin is significantly increased when prostate and breast cancer cells are stimulated with WNT3A. Interactions between SOX4 and plakoglobin were further enhanced by the nuclear export inhibitor leptomycin B (LMB), suggesting that plakoglobin promotes nuclear export of SOX4. The SOX4-plakoglobin complex affected the expression of Wnt pathway target genes and SOX4 downstream targets, such as <it>AXIN2</it>, <it>DICER1</it>, and <it>DHX9</it>. In addition, SOX4 DNA binding activity to the promoters of <it>DICER1</it>, <it>AXIN2</it>, <it>DHX9 </it>and <it>SOX4 </it>itself was reduced by conditions that promote SOX4-plakoglobin complex formation. Conditions that enhanced SOX4-plakoglobin interactions resulted in reduced transcriptional activity of β-catenin luciferase reporters.</p> <p>Conclusions</p> <p>These data suggest that this newly identified interaction between SOX4 and plakoglobin is inhibitory and provides new insights into the role of SOX4 in key pathways in cell proliferation, development, and cancer progression.</p>
url http://www.biomedcentral.com/1471-2121/12/50
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