Detrusor induction of miR-132/212 following bladder outlet obstruction: association with MeCP2 repression and cell viability.

Detrusor induction of miR-132/212 following bladder outlet obstruction: association with MeCP2 repression and cell viability.

The microRNAs (miRNAs) miR-132 and miR-212 have been found to regulate synaptic plasticity and cholinergic signaling and recent work has demonstrated roles outside of the CNS, including in smooth muscle. Here, we examined if miR-132 and miR-212 are induced in the urinary bladder following outlet obs...

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Main Authors: Mardjaneh Karbalaei Sadegh, Mari Ekman, Katarzyna Krawczyk, Daniel Svensson, Olga Göransson, Diana Dahan, Bengt-Olof Nilsson, Sebastian Albinsson, Bengt Uvelius, Karl Swärd
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4305303?pdf=render
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spelling doaj-d39c94093e2543eba600288a6a4cd13d2020-11-25T00:51:27ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01101e011678410.1371/journal.pone.0116784Detrusor induction of miR-132/212 following bladder outlet obstruction: association with MeCP2 repression and cell viability.Mardjaneh Karbalaei SadeghMari EkmanKatarzyna KrawczykDaniel SvenssonOlga GöranssonDiana DahanBengt-Olof NilssonSebastian AlbinssonBengt UveliusKarl SwärdThe microRNAs (miRNAs) miR-132 and miR-212 have been found to regulate synaptic plasticity and cholinergic signaling and recent work has demonstrated roles outside of the CNS, including in smooth muscle. Here, we examined if miR-132 and miR-212 are induced in the urinary bladder following outlet obstruction and whether this correlates with effects on gene expression and cell growth. Three to seven-fold induction of miR-132/212 was found at 10 days of obstruction and this was selective for the detrusor layer. We cross-referenced putative binding sites in the miR-132/212 promoter with transcription factors that were predicted to be active in the obstruction model. This suggested involvement of Creb and Ahr in miR-132/212 induction. Creb phosphorylation (S-133) was not increased, but the number of Ahr positive nuclei increased. Moreover, we found that serum stimulation and protein kinase C activation induced miR-132/212 in human detrusor cells. To identify miR-132/212 targets, we correlated the mRNA levels of validated targets with the miRNA levels. Significant correlations between miR-132/212 and MeCP2, Ep300, Pnkd and Jarid1a were observed, and the protein levels of MeCP2, Pnkd and Ache were reduced after obstruction. Reduction of Ache however closely matched a 90% reduction of synapse density arguing that its repression was unrelated to miR-132/212 induction. Importantly, transfection of antimirs and mimics in cultured detrusor cells increased and decreased, respectively, the number of cells and led to changes in MeCP2 expression. In all, these findings show that obstruction of the urethra increases miR-132 and miR-212 in the detrusor and suggests that this influences gene expression and limits cell growth.http://europepmc.org/articles/PMC4305303?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Mardjaneh Karbalaei Sadegh
Mari Ekman
Katarzyna Krawczyk
Daniel Svensson
Olga Göransson
Diana Dahan
Bengt-Olof Nilsson
Sebastian Albinsson
Bengt Uvelius
Karl Swärd
spellingShingle Mardjaneh Karbalaei Sadegh
Mari Ekman
Katarzyna Krawczyk
Daniel Svensson
Olga Göransson
Diana Dahan
Bengt-Olof Nilsson
Sebastian Albinsson
Bengt Uvelius
Karl Swärd
Detrusor induction of miR-132/212 following bladder outlet obstruction: association with MeCP2 repression and cell viability.
PLoS ONE
author_facet Mardjaneh Karbalaei Sadegh
Mari Ekman
Katarzyna Krawczyk
Daniel Svensson
Olga Göransson
Diana Dahan
Bengt-Olof Nilsson
Sebastian Albinsson
Bengt Uvelius
Karl Swärd
author_sort Mardjaneh Karbalaei Sadegh
title Detrusor induction of miR-132/212 following bladder outlet obstruction: association with MeCP2 repression and cell viability.
title_short Detrusor induction of miR-132/212 following bladder outlet obstruction: association with MeCP2 repression and cell viability.
title_full Detrusor induction of miR-132/212 following bladder outlet obstruction: association with MeCP2 repression and cell viability.
title_fullStr Detrusor induction of miR-132/212 following bladder outlet obstruction: association with MeCP2 repression and cell viability.
title_full_unstemmed Detrusor induction of miR-132/212 following bladder outlet obstruction: association with MeCP2 repression and cell viability.
title_sort detrusor induction of mir-132/212 following bladder outlet obstruction: association with mecp2 repression and cell viability.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description The microRNAs (miRNAs) miR-132 and miR-212 have been found to regulate synaptic plasticity and cholinergic signaling and recent work has demonstrated roles outside of the CNS, including in smooth muscle. Here, we examined if miR-132 and miR-212 are induced in the urinary bladder following outlet obstruction and whether this correlates with effects on gene expression and cell growth. Three to seven-fold induction of miR-132/212 was found at 10 days of obstruction and this was selective for the detrusor layer. We cross-referenced putative binding sites in the miR-132/212 promoter with transcription factors that were predicted to be active in the obstruction model. This suggested involvement of Creb and Ahr in miR-132/212 induction. Creb phosphorylation (S-133) was not increased, but the number of Ahr positive nuclei increased. Moreover, we found that serum stimulation and protein kinase C activation induced miR-132/212 in human detrusor cells. To identify miR-132/212 targets, we correlated the mRNA levels of validated targets with the miRNA levels. Significant correlations between miR-132/212 and MeCP2, Ep300, Pnkd and Jarid1a were observed, and the protein levels of MeCP2, Pnkd and Ache were reduced after obstruction. Reduction of Ache however closely matched a 90% reduction of synapse density arguing that its repression was unrelated to miR-132/212 induction. Importantly, transfection of antimirs and mimics in cultured detrusor cells increased and decreased, respectively, the number of cells and led to changes in MeCP2 expression. In all, these findings show that obstruction of the urethra increases miR-132 and miR-212 in the detrusor and suggests that this influences gene expression and limits cell growth.
url http://europepmc.org/articles/PMC4305303?pdf=render
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