Adhesion glycoprotein CD44 functions as an upstream regulator of a network connecting ERK, AKT and Hippo-YAP pathways in cancer progression

Targeted therapies are considered to be the future of cancer treatment. However, the mechanism through which intracellular signaling pathways coordinate to modulate oncogenesis remains to be elucidated. In this study, we describe a novel crosstalk among ERK, AKT and Hippo-YAP pathways, with CD44 as...

Descripción completa

Detalles Bibliográficos
Autores principales: Yu, Shiyi, Cai, Xiuxiu, Wu, Chenxi, Wu, Lele, Wang, Yuzhi, Liu, Yan, Yu, Zhenghong, Qin, Sheng, Ma, Fei, Thiery, Jean Paul, Chen, Liming
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2014
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4413630/
https://www.ncbi.nlm.nih.gov/pubmed/25605020
_version_ 1782368810627497984
author Yu, Shiyi
Cai, Xiuxiu
Wu, Chenxi
Wu, Lele
Wang, Yuzhi
Liu, Yan
Yu, Zhenghong
Qin, Sheng
Ma, Fei
Thiery, Jean Paul
Chen, Liming
author_facet Yu, Shiyi
Cai, Xiuxiu
Wu, Chenxi
Wu, Lele
Wang, Yuzhi
Liu, Yan
Yu, Zhenghong
Qin, Sheng
Ma, Fei
Thiery, Jean Paul
Chen, Liming
author_sort Yu, Shiyi
collection PubMed
description Targeted therapies are considered to be the future of cancer treatment. However, the mechanism through which intracellular signaling pathways coordinate to modulate oncogenesis remains to be elucidated. In this study, we describe a novel crosstalk among ERK, AKT and Hippo-YAP pathways, with CD44 as an upstream regulator. High cell density leads to activation of ERK and AKT but inactivation of YAP in cancer cells. CD44 modulates cell proliferation and cell cycle but not apoptosis. The expression and activity of cell cycle genes were cooperatively regulated by ERK, AKT and Hippo-YAP signaling pathways through CD44-mediated mechanisms. In addition, CD44 depletion abrogates cancer stem cell properties of tumor initiating cells. Taken together, we described a paradigm where CD44 functions as an upstream regulator sensing the extracellular environment to modulate ERK, AKT and Hippo-YAP pathways which cooperatively control downstream gene expression to modulate cell contact inhibition of proliferation, cell cycle progression and maintenance of tumor initiating cells. Our current study provides valuable information to design targeted therapeutic strategies in cancers.
format Online
Article
Text
id pubmed-4413630
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Impact Journals LLC
record_format MEDLINE/PubMed
spelling pubmed-44136302015-05-08 Adhesion glycoprotein CD44 functions as an upstream regulator of a network connecting ERK, AKT and Hippo-YAP pathways in cancer progression Yu, Shiyi Cai, Xiuxiu Wu, Chenxi Wu, Lele Wang, Yuzhi Liu, Yan Yu, Zhenghong Qin, Sheng Ma, Fei Thiery, Jean Paul Chen, Liming Oncotarget Research Paper Targeted therapies are considered to be the future of cancer treatment. However, the mechanism through which intracellular signaling pathways coordinate to modulate oncogenesis remains to be elucidated. In this study, we describe a novel crosstalk among ERK, AKT and Hippo-YAP pathways, with CD44 as an upstream regulator. High cell density leads to activation of ERK and AKT but inactivation of YAP in cancer cells. CD44 modulates cell proliferation and cell cycle but not apoptosis. The expression and activity of cell cycle genes were cooperatively regulated by ERK, AKT and Hippo-YAP signaling pathways through CD44-mediated mechanisms. In addition, CD44 depletion abrogates cancer stem cell properties of tumor initiating cells. Taken together, we described a paradigm where CD44 functions as an upstream regulator sensing the extracellular environment to modulate ERK, AKT and Hippo-YAP pathways which cooperatively control downstream gene expression to modulate cell contact inhibition of proliferation, cell cycle progression and maintenance of tumor initiating cells. Our current study provides valuable information to design targeted therapeutic strategies in cancers. Impact Journals LLC 2014-12-30 /pmc/articles/PMC4413630/ /pubmed/25605020 Text en Copyright: © 2015 Yu 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
Yu, Shiyi
Cai, Xiuxiu
Wu, Chenxi
Wu, Lele
Wang, Yuzhi
Liu, Yan
Yu, Zhenghong
Qin, Sheng
Ma, Fei
Thiery, Jean Paul
Chen, Liming
Adhesion glycoprotein CD44 functions as an upstream regulator of a network connecting ERK, AKT and Hippo-YAP pathways in cancer progression
title Adhesion glycoprotein CD44 functions as an upstream regulator of a network connecting ERK, AKT and Hippo-YAP pathways in cancer progression
title_full Adhesion glycoprotein CD44 functions as an upstream regulator of a network connecting ERK, AKT and Hippo-YAP pathways in cancer progression
title_fullStr Adhesion glycoprotein CD44 functions as an upstream regulator of a network connecting ERK, AKT and Hippo-YAP pathways in cancer progression
title_full_unstemmed Adhesion glycoprotein CD44 functions as an upstream regulator of a network connecting ERK, AKT and Hippo-YAP pathways in cancer progression
title_short Adhesion glycoprotein CD44 functions as an upstream regulator of a network connecting ERK, AKT and Hippo-YAP pathways in cancer progression
title_sort adhesion glycoprotein cd44 functions as an upstream regulator of a network connecting erk, akt and hippo-yap pathways in cancer progression
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4413630/
https://www.ncbi.nlm.nih.gov/pubmed/25605020
work_keys_str_mv AT yushiyi adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT caixiuxiu adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT wuchenxi adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT wulele adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT wangyuzhi adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT liuyan adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT yuzhenghong adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT qinsheng adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT mafei adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT thieryjeanpaul adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression
AT chenliming adhesionglycoproteincd44functionsasanupstreamregulatorofanetworkconnectingerkaktandhippoyappathwaysincancerprogression

Ejemplares similares