miR-31 targets ARID1A and enhances the oncogenicity and stemness of head and neck squamous cell carcinoma

Wen Cheng Lu; Chung Ji Liu; Hsi Feng Tu; Yu Tung Chung; Cheng Chieh Yang; Shou Yen Kao; Kuo Wei Chang; Shu Chun Lin

doi:10.18632/oncotarget.11138

miR-31 targets ARID1A and enhances the oncogenicity and stemness of head and neck squamous cell carcinoma

Wen Cheng Lu, Chung Ji Liu, Hsi Feng Tu, Yu Tung Chung, Cheng Chieh Yang, Shou Yen Kao, Kuo Wei Chang^*, Shu Chun Lin

^*Corresponding author for this work

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

44 Scopus citations

Abstract

miR-31 is oncogenic for head and neck squamous cell carcinoma (HNSCC). Proteins containing the AT-rich interacting domain (ARID) modulate the accessibility of chromatin to the transcription machinery needed for gene expression. In this study, we showed that miR-31 was able to target ARID1A in HNSCC. HNSCC tumors had an inverse miR-31 and ARID1A expression. miR-31 associated oncogenicities were rescued by ARID1A expression in HNSCC cells. Furthermore, ARID1A repressed the stemness properties and transcriptional activity of Nanog/OCT4/Sox2/EpCAM via the protein's affinity for AT-rich sites within promoters. HNSCC patients with tumors having high level of miR-31 expression and high levels of Nanog/OCT4/Sox2/EpCAM expression, together with low level of ARID1A expression, were found to have the worst survival. This study provides novel mechanistic clues demonstrating that miR- 31 inhibits ARID1A and that this enriches the oncogenicity and stemness of HNSCC.

Original language	English
Pages (from-to)	57254-57267
Number of pages	14
Journal	Oncotarget
Volume	7
Issue number	35
DOIs	https://doi.org/10.18632/oncotarget.11138
State	Published - 2016

Keywords

ARID1A
Cancer
MiR-31
Stem cell
Suppressor

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.18632/oncotarget.11138

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title = "miR-31 targets ARID1A and enhances the oncogenicity and stemness of head and neck squamous cell carcinoma",

abstract = "miR-31 is oncogenic for head and neck squamous cell carcinoma (HNSCC). Proteins containing the AT-rich interacting domain (ARID) modulate the accessibility of chromatin to the transcription machinery needed for gene expression. In this study, we showed that miR-31 was able to target ARID1A in HNSCC. HNSCC tumors had an inverse miR-31 and ARID1A expression. miR-31 associated oncogenicities were rescued by ARID1A expression in HNSCC cells. Furthermore, ARID1A repressed the stemness properties and transcriptional activity of Nanog/OCT4/Sox2/EpCAM via the protein's affinity for AT-rich sites within promoters. HNSCC patients with tumors having high level of miR-31 expression and high levels of Nanog/OCT4/Sox2/EpCAM expression, together with low level of ARID1A expression, were found to have the worst survival. This study provides novel mechanistic clues demonstrating that miR- 31 inhibits ARID1A and that this enriches the oncogenicity and stemness of HNSCC.",

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author = "Lu, {Wen Cheng} and Liu, {Chung Ji} and Tu, {Hsi Feng} and Chung, {Yu Tung} and Yang, {Cheng Chieh} and Kao, {Shou Yen} and Chang, {Kuo Wei} and Lin, {Shu Chun}",

note = "Funding Information: This study was supported by grants MOST102-2628-B-010-011-MY3 and MOST103-2314-B-010-020-MY3 from Ministry of Science and Technology and Welfare Surcharge on tobacco products grant number MOHW105-TDU-B-211-134-003 from Ministry of Health and Welfare for Excellence for Cancer Research",

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language = "English",

volume = "7",

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TY - JOUR

T1 - miR-31 targets ARID1A and enhances the oncogenicity and stemness of head and neck squamous cell carcinoma

AU - Lu, Wen Cheng

AU - Liu, Chung Ji

AU - Tu, Hsi Feng

AU - Chung, Yu Tung

AU - Yang, Cheng Chieh

AU - Kao, Shou Yen

AU - Chang, Kuo Wei

AU - Lin, Shu Chun

N1 - Funding Information: This study was supported by grants MOST102-2628-B-010-011-MY3 and MOST103-2314-B-010-020-MY3 from Ministry of Science and Technology and Welfare Surcharge on tobacco products grant number MOHW105-TDU-B-211-134-003 from Ministry of Health and Welfare for Excellence for Cancer Research

PY - 2016

Y1 - 2016

N2 - miR-31 is oncogenic for head and neck squamous cell carcinoma (HNSCC). Proteins containing the AT-rich interacting domain (ARID) modulate the accessibility of chromatin to the transcription machinery needed for gene expression. In this study, we showed that miR-31 was able to target ARID1A in HNSCC. HNSCC tumors had an inverse miR-31 and ARID1A expression. miR-31 associated oncogenicities were rescued by ARID1A expression in HNSCC cells. Furthermore, ARID1A repressed the stemness properties and transcriptional activity of Nanog/OCT4/Sox2/EpCAM via the protein's affinity for AT-rich sites within promoters. HNSCC patients with tumors having high level of miR-31 expression and high levels of Nanog/OCT4/Sox2/EpCAM expression, together with low level of ARID1A expression, were found to have the worst survival. This study provides novel mechanistic clues demonstrating that miR- 31 inhibits ARID1A and that this enriches the oncogenicity and stemness of HNSCC.

AB - miR-31 is oncogenic for head and neck squamous cell carcinoma (HNSCC). Proteins containing the AT-rich interacting domain (ARID) modulate the accessibility of chromatin to the transcription machinery needed for gene expression. In this study, we showed that miR-31 was able to target ARID1A in HNSCC. HNSCC tumors had an inverse miR-31 and ARID1A expression. miR-31 associated oncogenicities were rescued by ARID1A expression in HNSCC cells. Furthermore, ARID1A repressed the stemness properties and transcriptional activity of Nanog/OCT4/Sox2/EpCAM via the protein's affinity for AT-rich sites within promoters. HNSCC patients with tumors having high level of miR-31 expression and high levels of Nanog/OCT4/Sox2/EpCAM expression, together with low level of ARID1A expression, were found to have the worst survival. This study provides novel mechanistic clues demonstrating that miR- 31 inhibits ARID1A and that this enriches the oncogenicity and stemness of HNSCC.

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KW - Cancer

KW - MiR-31

KW - Stem cell

KW - Suppressor

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miR-31 targets ARID1A and enhances the oncogenicity and stemness of head and neck squamous cell carcinoma

Abstract

Keywords

UN SDGs

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