Long non-coding RNA SDCBP2-AS1 delays the progression of ovarian cancer via microRNA-100-5p-targeted EPDR1
Abstract Background Dysregulation of long non-coding RNAs has been implied to connect with cancer progression. This research was to decipher the mechanism of long non-coding RNA SDCBP2-AS1 in ovarian cancer (OC) through regulation of microRNA (miR)-100-5p and ependymin-related protein 1 (EPDR1). Met...
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doaj-ce7bde87bb254dc09371dc7efecbc6cf2021-07-11T11:41:29ZengBMCWorld Journal of Surgical Oncology1477-78192021-07-011911910.1186/s12957-021-02295-2Long non-coding RNA SDCBP2-AS1 delays the progression of ovarian cancer via microRNA-100-5p-targeted EPDR1Xiu Liu0Chanyuan Liu1Aijun Zhang2Qi Wang3Jiao Ge4Qunying Li5Jinlei Xiao6Wuhan Wuchang Hospital, Wuhan University of Science and TechnologyWuhan Wuchang Hospital, Wuhan University of Science and TechnologyWuhan Wuchang Hospital, Wuhan University of Science and TechnologyWuhan Wuchang Hospital, Wuhan University of Science and TechnologyWuhan Wuchang Hospital, Wuhan University of Science and TechnologyWuhan Wuchang Hospital, Wuhan University of Science and TechnologyWuhan Wuchang Hospital, Wuhan University of Science and TechnologyAbstract Background Dysregulation of long non-coding RNAs has been implied to connect with cancer progression. This research was to decipher the mechanism of long non-coding RNA SDCBP2-AS1 in ovarian cancer (OC) through regulation of microRNA (miR)-100-5p and ependymin-related protein 1 (EPDR1). Methods LncRNA SDCBP2-AS1 and EPDR1 levels in OC were assessed by Gene Expression Profiling Interactive Analysis. lncRNA SDCBP2-AS1, miR-100-5p, and EPDR1 levels in OC tissues and cells were determined. SKOV3 and A2780 cells were transfected with lncRNA SDCBP2-AS1, miR-100-5p, and EPDR1-related plasmids or sequences, and then their functions in cell viability, apoptosis, migration, and invasion were evaluated. The interplay of lncRNA SDCBP2-AS1, miR-100-5p, and EPDR1 was clarified. Results LncRNA SDCBP2-AS1 and EPDR1 levels were suppressed whilst miR-100-5p level was elevated in OC. After upregulating lncRNA SDCBP2-AS1 or EPDR1, viability, migration, and invasion of OC cells were impaired, and apoptosis rate was increased. Downregulating EPDR1 or upregulating miR-100-5p partially mitigated upregulated lncRNA SDCBP2-AS1-induced impacts on the biological functions of OC cells. LncRNA SDCBP2-AS1 sponged miR-100-5p, and EPDR1 was targeted by miR-100-5p. Conclusion It is illustrated that lncRNA SDCBP2-AS1 regulates EPDR1 by sponge adsorption of miR-100-5p to inhibit the progression of OC.https://doi.org/10.1186/s12957-021-02295-2Ovarian cancerLong non-coding RNA SDCBP2-AS1MicroRNA-100-5pEpendymin-related protein 1ViabilityApoptosis |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Xiu Liu Chanyuan Liu Aijun Zhang Qi Wang Jiao Ge Qunying Li Jinlei Xiao |
spellingShingle |
Xiu Liu Chanyuan Liu Aijun Zhang Qi Wang Jiao Ge Qunying Li Jinlei Xiao Long non-coding RNA SDCBP2-AS1 delays the progression of ovarian cancer via microRNA-100-5p-targeted EPDR1 World Journal of Surgical Oncology Ovarian cancer Long non-coding RNA SDCBP2-AS1 MicroRNA-100-5p Ependymin-related protein 1 Viability Apoptosis |
author_facet |
Xiu Liu Chanyuan Liu Aijun Zhang Qi Wang Jiao Ge Qunying Li Jinlei Xiao |
author_sort |
Xiu Liu |
title |
Long non-coding RNA SDCBP2-AS1 delays the progression of ovarian cancer via microRNA-100-5p-targeted EPDR1 |
title_short |
Long non-coding RNA SDCBP2-AS1 delays the progression of ovarian cancer via microRNA-100-5p-targeted EPDR1 |
title_full |
Long non-coding RNA SDCBP2-AS1 delays the progression of ovarian cancer via microRNA-100-5p-targeted EPDR1 |
title_fullStr |
Long non-coding RNA SDCBP2-AS1 delays the progression of ovarian cancer via microRNA-100-5p-targeted EPDR1 |
title_full_unstemmed |
Long non-coding RNA SDCBP2-AS1 delays the progression of ovarian cancer via microRNA-100-5p-targeted EPDR1 |
title_sort |
long non-coding rna sdcbp2-as1 delays the progression of ovarian cancer via microrna-100-5p-targeted epdr1 |
publisher |
BMC |
series |
World Journal of Surgical Oncology |
issn |
1477-7819 |
publishDate |
2021-07-01 |
description |
Abstract Background Dysregulation of long non-coding RNAs has been implied to connect with cancer progression. This research was to decipher the mechanism of long non-coding RNA SDCBP2-AS1 in ovarian cancer (OC) through regulation of microRNA (miR)-100-5p and ependymin-related protein 1 (EPDR1). Methods LncRNA SDCBP2-AS1 and EPDR1 levels in OC were assessed by Gene Expression Profiling Interactive Analysis. lncRNA SDCBP2-AS1, miR-100-5p, and EPDR1 levels in OC tissues and cells were determined. SKOV3 and A2780 cells were transfected with lncRNA SDCBP2-AS1, miR-100-5p, and EPDR1-related plasmids or sequences, and then their functions in cell viability, apoptosis, migration, and invasion were evaluated. The interplay of lncRNA SDCBP2-AS1, miR-100-5p, and EPDR1 was clarified. Results LncRNA SDCBP2-AS1 and EPDR1 levels were suppressed whilst miR-100-5p level was elevated in OC. After upregulating lncRNA SDCBP2-AS1 or EPDR1, viability, migration, and invasion of OC cells were impaired, and apoptosis rate was increased. Downregulating EPDR1 or upregulating miR-100-5p partially mitigated upregulated lncRNA SDCBP2-AS1-induced impacts on the biological functions of OC cells. LncRNA SDCBP2-AS1 sponged miR-100-5p, and EPDR1 was targeted by miR-100-5p. Conclusion It is illustrated that lncRNA SDCBP2-AS1 regulates EPDR1 by sponge adsorption of miR-100-5p to inhibit the progression of OC. |
topic |
Ovarian cancer Long non-coding RNA SDCBP2-AS1 MicroRNA-100-5p Ependymin-related protein 1 Viability Apoptosis |
url |
https://doi.org/10.1186/s12957-021-02295-2 |
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