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Citations to this article

CD44 splice isoform switching in human and mouse epithelium is essential for epithelial-mesenchymal transition and breast cancer progression
Rhonda L. Brown, … , Jing Yang, Chonghui Cheng
Rhonda L. Brown, … , Jing Yang, Chonghui Cheng
Published February 14, 2011
Citation Information: J Clin Invest. 2011;121(3):1064-1074. https://doi.org/10.1172/JCI44540.
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Research Article Oncology Article has an altmetric score of 7

CD44 splice isoform switching in human and mouse epithelium is essential for epithelial-mesenchymal transition and breast cancer progression

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Abstract

Epithelial-mesenchymal transition (EMT) is a tightly regulated process that is critical for embryogenesis but is abnormally activated during cancer metastasis and recurrence. Here we show that a switch in CD44 alternative splicing is required for EMT. Using both in vitro and in vivo systems, we have demonstrated a shift in CD44 expression from variant isoforms (CD44v) to the standard isoform (CD44s) during EMT. This isoform switch to CD44s was essential for cells to undergo EMT and was required for the formation of breast tumors that display EMT characteristics in mice. Mechanistically, the splicing factor epithelial splicing regulatory protein 1 (ESRP1) controlled the CD44 isoform switch and was critical for regulating the EMT phenotype. Additionally, the CD44s isoform activated Akt signaling, providing a mechanistic link to a key pathway that drives EMT. Finally, CD44s expression was upregulated in high-grade human breast tumors and was correlated with the level of the mesenchymal marker N-cadherin in these tumors. Together, our data suggest that regulation of CD44 alternative splicing causally contributes to EMT and breast cancer progression.

Authors

Rhonda L. Brown, Lauren M. Reinke, Marin S. Damerow, Denise Perez, Lewis A. Chodosh, Jing Yang, Chonghui Cheng

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Total citations by year

Year: 2025 2024 2023 2022 2021 2020 2019 2018 2017 2016 2015 2014 2013 2012 2011 2009 Total
Citations: 9 25 28 36 23 31 29 26 27 22 29 23 22 19 9 1 359
Citation information
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Citations to this article in year 2011 (9)

Title and authors Publication Year
ERK1/2 regulation of CD44 modulates oral cancer aggressiveness
NP Judd, AE Winkler, O Murillo-Sauca, JJ Brotman, JH Law, JS Lewis, GP Dunn, JD Bui, JB Sunwoo, R Uppaluri
Cancer research 2011
An EMT–Driven Alternative Splicing Program Occurs in Human Breast Cancer and Modulates Cellular Phenotype
IM Shapiro, AW Cheng, NC Flytzanis, M Balsamo, JS Condeelis, MH Oktay, CB Burge, FB Gertler
PLoS genetics 2011
Functional consequences of developmentally regulated alternative splicing
A Kalsotra, TA Cooper
Nature reviews. Genetics 2011
Soluble CD44 Interacts with Intermediate Filament Protein Vimentin on Endothelial Cell Surface
T Päll, A Pink, L Kasak, M Turkina, W Anderson, A Valkna, P Kogerman
PloS one 2011
The 'alternative' EMT switch
P Klingbeil, CM Isacke
Breast Cancer Research 2011
CD44 Upregulation in E-Cadherin-Negative Esophageal Cancers Results in Cell Invasion
GF le Bras, GL Allison, NF Richards, SS Ansari, MK Washington, CD Andl
PloS one 2011
CD44 isoforms are heterogeneously expressed in breast cancer and correlate with tumor subtypes and cancer stem cell markers
E Olsson, G Honeth, PO Bendahl, LH Saal, S Gruvberger-Saal, M Ringnér, J Vallon-Christersson, G Jönsson, K Holm, K Lövgren, M Fernö, D Grabau, A Borg, C Hegardt
BMC Cancer 2011
Contribution of epithelial-to-mesenchymal transition and cancer stem cells to pancreatic cancer progression
SB Krantz, MA Shields, S Dangi-Garimella, HG Munshi, DJ Bentrem
The Journal of surgical research 2011
Cancer stem cells and side population cells in breast cancer and metastasis
KM Britton, JA Kirby, TW Lennard, AP Meeson
Cancers 2011

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