LINC01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating KLF4

LINC01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating KLF4

Background: In recent years, a large number of studies have shown that differentially expressed lncRNAs in tumors are capable of inducing tumorigenesis and promoting tumor development. However, the role of LINC01210 in OC still remains unclear. Methods: Relative levels of LINC01210 and KLF4 in OC ti...

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Main Authors: Chu Zhang, Jie Liu, Yang Zhang, Chengyan Luo, Tong Zhu, Rongrong Zhang, Ruiqin Yao
Format: Article
Language:English
Published: Elsevier 2019-11-01
Series:Biomedicine & Pharmacotherapy
Subjects:
Ovarian cancer
LINC01210
KLF4
Proliferation
Migration
Invasion
Online Access:http://www.sciencedirect.com/science/article/pii/S0753332219333165
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spelling doaj-3ba4e4555ef344dd919b3d059774f0332021-05-20T07:38:58ZengElsevierBiomedicine & Pharmacotherapy0753-33222019-11-01119LINC01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating KLF4Chu Zhang0Jie Liu1Yang Zhang2Chengyan Luo3Tong Zhu4Rongrong Zhang5Ruiqin Yao6Department of Reproduction Center, Xuzhou Maternity and Child Health Care Hospital, Xuzhou, PR China; Corresponding author at: Department of Reproduction Center, Xuzhou Maternity and Child Health Care Hospital, NO. 46 Heping Road, Xuzhou, 221000, China.Department of Reproduction Center, Xuzhou Maternity and Child Health Care Hospital, Xuzhou, PR ChinaXuzhou Prison Hospital of Jiangsu Province, Xuzhou, PR ChinaDepartment of Gynecology, The First Affiliated Hospital of Nanjing Medical University, Nanjing, Jiangsu Province, PR ChinaDepartment of Reproduction Center, Xuzhou Maternity and Child Health Care Hospital, Xuzhou, PR ChinaDepartment of Reproduction Center, Xuzhou Maternity and Child Health Care Hospital, Xuzhou, PR ChinaDepartment of Cell Biology and Neurobiology, Xuzhou Key Laboratory of Neurobiology, Xuzhou Medical University, Xuzhou, PR China; Corresponding author at: Department of Cell Biology and Neurobiology, Xuzhou Key Laboratory of Neurobiology, Xuzhou Medical University, NO. 209 Tongshan Road, Xuzhou, 221000, China.Background: In recent years, a large number of studies have shown that differentially expressed lncRNAs in tumors are capable of inducing tumorigenesis and promoting tumor development. However, the role of LINC01210 in OC still remains unclear. Methods: Relative levels of LINC01210 and KLF4 in OC tissues containing in the GSE40595 dataset and those collected in our hospital were determined. Prognostic potential of LINC01210 in OC was evaluated by Kaplan-Meier method. Correlation between expression levels of LINC01210 and KLF4 was assessed by Spearman correlation test. After silence of LINC01210 in A2780 and HO8910 cells, changes in proliferative, migratory and invasive abilities were examined. Moreover, the interaction between LINC01210 and KLF4 was explored by RIP and ChIP. Rescue experiments were conducted to uncover the involvement of KLF4 in LINC01210-regulated OC progression. Results: LINC01210 was upregulated in OC tissues and KLF4 was downregulated. LINC01210 level was higher in OC patients with metastases or advanced stage. Besides, its level was negatively correlated to DFS (disease-free survival) and OS (overall survival) of OC patients. Silence of LINC01210 attenuated proliferative, migratory and invasive abilities in A2780 and HO8910 cells. Through analyzing the GSE40595 dataset, LINC01210 was found to be negatively linked to KLF4. RIP assay further verified the interaction between LINC01210 and KLF4. Knockdown of LINC01210 markedly decreased the recruitment ability of EZH2 to KLF4. Importantly, silence of KLF4 could reverse regulatory effects of LINC01210 on cellular behaviors of OC. Conclusions: LINC01210 is upregulated in OC and predicts a poor prognosis. It accelerates proliferation, invasion and migration in OC cells through epigenetically downregulating KLF4.http://www.sciencedirect.com/science/article/pii/S0753332219333165Ovarian cancerLINC01210KLF4ProliferationMigrationInvasion
collection DOAJ
language English
format Article
sources DOAJ
author Chu Zhang
Jie Liu
Yang Zhang
Chengyan Luo
Tong Zhu
Rongrong Zhang
Ruiqin Yao
spellingShingle Chu Zhang
Jie Liu
Yang Zhang
Chengyan Luo
Tong Zhu
Rongrong Zhang
Ruiqin Yao
LINC01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating KLF4
Biomedicine & Pharmacotherapy
Ovarian cancer
LINC01210
KLF4
Proliferation
Migration
Invasion
author_facet Chu Zhang
Jie Liu
Yang Zhang
Chengyan Luo
Tong Zhu
Rongrong Zhang
Ruiqin Yao
author_sort Chu Zhang
title LINC01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating KLF4
title_short LINC01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating KLF4
title_full LINC01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating KLF4
title_fullStr LINC01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating KLF4
title_full_unstemmed LINC01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating KLF4
title_sort linc01210 accelerates proliferation, invasion and migration in ovarian cancer through epigenetically downregulating klf4
publisher Elsevier
series Biomedicine & Pharmacotherapy
issn 0753-3322
publishDate 2019-11-01
description Background: In recent years, a large number of studies have shown that differentially expressed lncRNAs in tumors are capable of inducing tumorigenesis and promoting tumor development. However, the role of LINC01210 in OC still remains unclear. Methods: Relative levels of LINC01210 and KLF4 in OC tissues containing in the GSE40595 dataset and those collected in our hospital were determined. Prognostic potential of LINC01210 in OC was evaluated by Kaplan-Meier method. Correlation between expression levels of LINC01210 and KLF4 was assessed by Spearman correlation test. After silence of LINC01210 in A2780 and HO8910 cells, changes in proliferative, migratory and invasive abilities were examined. Moreover, the interaction between LINC01210 and KLF4 was explored by RIP and ChIP. Rescue experiments were conducted to uncover the involvement of KLF4 in LINC01210-regulated OC progression. Results: LINC01210 was upregulated in OC tissues and KLF4 was downregulated. LINC01210 level was higher in OC patients with metastases or advanced stage. Besides, its level was negatively correlated to DFS (disease-free survival) and OS (overall survival) of OC patients. Silence of LINC01210 attenuated proliferative, migratory and invasive abilities in A2780 and HO8910 cells. Through analyzing the GSE40595 dataset, LINC01210 was found to be negatively linked to KLF4. RIP assay further verified the interaction between LINC01210 and KLF4. Knockdown of LINC01210 markedly decreased the recruitment ability of EZH2 to KLF4. Importantly, silence of KLF4 could reverse regulatory effects of LINC01210 on cellular behaviors of OC. Conclusions: LINC01210 is upregulated in OC and predicts a poor prognosis. It accelerates proliferation, invasion and migration in OC cells through epigenetically downregulating KLF4.
topic Ovarian cancer
LINC01210
KLF4
Proliferation
Migration
Invasion
url http://www.sciencedirect.com/science/article/pii/S0753332219333165
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