LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values

Gespeichert in:

Bibliographische Detailangaben
Zeitschriftentitel:	Bioscience Reports
Personen und Körperschaften:	Chen, Zhongjun, Zhen, Ming, Zhou, Jiajie
In:	Bioscience Reports, 39, 2019, 3
Format:	E-Article
Sprache:	Englisch
veröffentlicht:	Portland Press Ltd.
Schlagwörter:	Cell Biology Molecular Biology Biochemistry Biophysics

author_facet	Chen, Zhongjun Zhen, Ming Zhou, Jiajie Chen, Zhongjun Zhen, Ming Zhou, Jiajie
author	Chen, Zhongjun Zhen, Ming Zhou, Jiajie
spellingShingle	Chen, Zhongjun Zhen, Ming Zhou, Jiajie Bioscience Reports LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values Cell Biology Molecular Biology Biochemistry Biophysics
author_sort	chen, zhongjun
spelling	Chen, Zhongjun Zhen, Ming Zhou, Jiajie 0144-8463 1573-4935 Portland Press Ltd. Cell Biology Molecular Biology Biochemistry Biophysics http://dx.doi.org/10.1042/bsr20182097 <jats:title>Abstract</jats:title> <jats:p>Long non-coding RNA (LncRNA) BRE-AS1 has recently proven to be a tumor suppressor in lung cancer. The present study aimed to investigate the involvement of lncRNA BRE-AS1 in prostate carcinoma (PC). In the present study we found that plasma BRE-AS1 and miR-145-5p were both down-regulated in PC patients than in healthy controls. Down-regulation of BRE-AS1 and miR-145-5p effectively distinguished early-stage PC patients from healthy controls. A significant and positive correlation between BRE-AS1 and miR-145–5p was only found in PC patients. BRE-AS1 overexpression mediated miR-145-5p up-regulation in PC cells, while miR-145-5p overexpression did not significantly affect BRE-AS1. Overexpression of BRE-AS1 and miR-145-5p led to inhibited proliferation and promoted apoptosis of PC cells. miR-145-5p inhibitor attenuated the effects of BRE-AS1 overexpression on cancer cell behaviors. Therefore, lncRNA BRE-AS1 may regulate cancer cell proliferation and apoptosis in PC by interacting with miR-145-5p.</jats:p> LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values Bioscience Reports
doi_str_mv	10.1042/bsr20182097
facet_avail	Online Free
finc_class_facet	Biologie Chemie und Pharmazie Physik
format	ElectronicArticle
fullrecord	blob:ai-49-aHR0cDovL2R4LmRvaS5vcmcvMTAuMTA0Mi9ic3IyMDE4MjA5Nw
id	ai-49-aHR0cDovL2R4LmRvaS5vcmcvMTAuMTA0Mi9ic3IyMDE4MjA5Nw
institution	DE-D275 DE-Bn3 DE-Brt1 DE-Zwi2 DE-D161 DE-Gla1 DE-Zi4 DE-15 DE-Pl11 DE-Rs1 DE-105 DE-14 DE-Ch1 DE-L229
imprint	Portland Press Ltd., 2019
imprint_str_mv	Portland Press Ltd., 2019
issn	0144-8463 1573-4935
issn_str_mv	0144-8463 1573-4935
language	English
mega_collection	Portland Press Ltd. (CrossRef)
match_str	chen2019lncrnabreas1interactswithmir1455ptoregulatecancercellproliferationandapoptosisinprostatecarcinomaandhasearlydiagnosticvalues
publishDateSort	2019
publisher	Portland Press Ltd.
recordtype	ai
record_format	ai
series	Bioscience Reports
source_id	49
title	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_unstemmed	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_full	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_fullStr	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_full_unstemmed	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_short	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_sort	lncrna bre-as1 interacts with mir-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
topic	Cell Biology Molecular Biology Biochemistry Biophysics
url	http://dx.doi.org/10.1042/bsr20182097
publishDate	2019
physical
description	<jats:title>Abstract</jats:title> <jats:p>Long non-coding RNA (LncRNA) BRE-AS1 has recently proven to be a tumor suppressor in lung cancer. The present study aimed to investigate the involvement of lncRNA BRE-AS1 in prostate carcinoma (PC). In the present study we found that plasma BRE-AS1 and miR-145-5p were both down-regulated in PC patients than in healthy controls. Down-regulation of BRE-AS1 and miR-145-5p effectively distinguished early-stage PC patients from healthy controls. A significant and positive correlation between BRE-AS1 and miR-145–5p was only found in PC patients. BRE-AS1 overexpression mediated miR-145-5p up-regulation in PC cells, while miR-145-5p overexpression did not significantly affect BRE-AS1. Overexpression of BRE-AS1 and miR-145-5p led to inhibited proliferation and promoted apoptosis of PC cells. miR-145-5p inhibitor attenuated the effects of BRE-AS1 overexpression on cancer cell behaviors. Therefore, lncRNA BRE-AS1 may regulate cancer cell proliferation and apoptosis in PC by interacting with miR-145-5p.</jats:p>
container_issue	3
container_start_page	0
container_title	Bioscience Reports
container_volume	39
format_de105	Article, E-Article
format_de14	Article, E-Article
format_de15	Article, E-Article
format_de520	Article, E-Article
format_de540	Article, E-Article
format_dech1	Article, E-Article
format_ded117	Article, E-Article
format_degla1	E-Article
format_del152	Buch
format_del189	Article, E-Article
format_dezi4	Article
format_dezwi2	Article, E-Article
format_finc	Article, E-Article
format_nrw	Article, E-Article
_version_	1792331200889618443
geogr_code	not assigned
last_indexed	2024-03-01T13:37:12.423Z
geogr_code_person	not assigned
openURL	url_ver=Z39.88-2004&ctx_ver=Z39.88-2004&ctx_enc=info%3Aofi%2Fenc%3AUTF-8&rfr_id=info%3Asid%2Fvufind.svn.sourceforge.net%3Agenerator&rft.title=LncRNA+BRE-AS1+interacts+with+miR-145-5p+to+regulate+cancer+cell+proliferation+and+apoptosis+in+prostate+carcinoma+and+has+early+diagnostic+values&rft.date=2019-03-29&genre=article&issn=1573-4935&volume=39&issue=3&jtitle=Bioscience+Reports&atitle=LncRNA+BRE-AS1+interacts+with+miR-145-5p+to+regulate+cancer+cell+proliferation+and+apoptosis+in+prostate+carcinoma+and+has+early+diagnostic+values&aulast=Zhou&aufirst=Jiajie&rft_id=info%3Adoi%2F10.1042%2Fbsr20182097&rft.language%5B0%5D=eng
SOLR
_version_	1792331200889618443
author	Chen, Zhongjun, Zhen, Ming, Zhou, Jiajie
author_facet	Chen, Zhongjun, Zhen, Ming, Zhou, Jiajie, Chen, Zhongjun, Zhen, Ming, Zhou, Jiajie
author_sort	chen, zhongjun
container_issue	3
container_start_page	0
container_title	Bioscience Reports
container_volume	39
description	<jats:title>Abstract</jats:title> <jats:p>Long non-coding RNA (LncRNA) BRE-AS1 has recently proven to be a tumor suppressor in lung cancer. The present study aimed to investigate the involvement of lncRNA BRE-AS1 in prostate carcinoma (PC). In the present study we found that plasma BRE-AS1 and miR-145-5p were both down-regulated in PC patients than in healthy controls. Down-regulation of BRE-AS1 and miR-145-5p effectively distinguished early-stage PC patients from healthy controls. A significant and positive correlation between BRE-AS1 and miR-145–5p was only found in PC patients. BRE-AS1 overexpression mediated miR-145-5p up-regulation in PC cells, while miR-145-5p overexpression did not significantly affect BRE-AS1. Overexpression of BRE-AS1 and miR-145-5p led to inhibited proliferation and promoted apoptosis of PC cells. miR-145-5p inhibitor attenuated the effects of BRE-AS1 overexpression on cancer cell behaviors. Therefore, lncRNA BRE-AS1 may regulate cancer cell proliferation and apoptosis in PC by interacting with miR-145-5p.</jats:p>
doi_str_mv	10.1042/bsr20182097
facet_avail	Online, Free
finc_class_facet	Biologie, Chemie und Pharmazie, Physik
format	ElectronicArticle
format_de105	Article, E-Article
format_de14	Article, E-Article
format_de15	Article, E-Article
format_de520	Article, E-Article
format_de540	Article, E-Article
format_dech1	Article, E-Article
format_ded117	Article, E-Article
format_degla1	E-Article
format_del152	Buch
format_del189	Article, E-Article
format_dezi4	Article
format_dezwi2	Article, E-Article
format_finc	Article, E-Article
format_nrw	Article, E-Article
geogr_code	not assigned
geogr_code_person	not assigned
id	ai-49-aHR0cDovL2R4LmRvaS5vcmcvMTAuMTA0Mi9ic3IyMDE4MjA5Nw
imprint	Portland Press Ltd., 2019
imprint_str_mv	Portland Press Ltd., 2019
institution	DE-D275, DE-Bn3, DE-Brt1, DE-Zwi2, DE-D161, DE-Gla1, DE-Zi4, DE-15, DE-Pl11, DE-Rs1, DE-105, DE-14, DE-Ch1, DE-L229
issn	0144-8463, 1573-4935
issn_str_mv	0144-8463, 1573-4935
language	English
last_indexed	2024-03-01T13:37:12.423Z
match_str	chen2019lncrnabreas1interactswithmir1455ptoregulatecancercellproliferationandapoptosisinprostatecarcinomaandhasearlydiagnosticvalues
mega_collection	Portland Press Ltd. (CrossRef)
physical
publishDate	2019
publishDateSort	2019
publisher	Portland Press Ltd.
record_format	ai
recordtype	ai
series	Bioscience Reports
source_id	49
spelling	Chen, Zhongjun Zhen, Ming Zhou, Jiajie 0144-8463 1573-4935 Portland Press Ltd. Cell Biology Molecular Biology Biochemistry Biophysics http://dx.doi.org/10.1042/bsr20182097 <jats:title>Abstract</jats:title> <jats:p>Long non-coding RNA (LncRNA) BRE-AS1 has recently proven to be a tumor suppressor in lung cancer. The present study aimed to investigate the involvement of lncRNA BRE-AS1 in prostate carcinoma (PC). In the present study we found that plasma BRE-AS1 and miR-145-5p were both down-regulated in PC patients than in healthy controls. Down-regulation of BRE-AS1 and miR-145-5p effectively distinguished early-stage PC patients from healthy controls. A significant and positive correlation between BRE-AS1 and miR-145–5p was only found in PC patients. BRE-AS1 overexpression mediated miR-145-5p up-regulation in PC cells, while miR-145-5p overexpression did not significantly affect BRE-AS1. Overexpression of BRE-AS1 and miR-145-5p led to inhibited proliferation and promoted apoptosis of PC cells. miR-145-5p inhibitor attenuated the effects of BRE-AS1 overexpression on cancer cell behaviors. Therefore, lncRNA BRE-AS1 may regulate cancer cell proliferation and apoptosis in PC by interacting with miR-145-5p.</jats:p> LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values Bioscience Reports
spellingShingle	Chen, Zhongjun, Zhen, Ming, Zhou, Jiajie, Bioscience Reports, LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values, Cell Biology, Molecular Biology, Biochemistry, Biophysics
title	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_full	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_fullStr	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_full_unstemmed	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_short	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_sort	lncrna bre-as1 interacts with mir-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
title_unstemmed	LncRNA BRE-AS1 interacts with miR-145-5p to regulate cancer cell proliferation and apoptosis in prostate carcinoma and has early diagnostic values
topic	Cell Biology, Molecular Biology, Biochemistry, Biophysics
url	http://dx.doi.org/10.1042/bsr20182097