Expression of stretch-activated two-pore potassium channels in human myometrium in pregnancy and labor.
We tested the hypothesis that the stretch-activated, four-transmembrane domain, two pore potassium channels (K2P), TREK-1 and TRAAK are gestationally-regulated in human myometrium and contribute to uterine relaxation during pregnancy until labor.We determined the gene and protein expression of K2P c...
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2010-08-01
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doaj-5a6ca33bdca34f8493e040822c36cfba2020-11-25T01:17:14ZengPublic Library of Science (PLoS)PLoS ONE1932-62032010-08-0158e1237210.1371/journal.pone.0012372Expression of stretch-activated two-pore potassium channels in human myometrium in pregnancy and labor.Iain L O BuxtonCherie A SingerJennifer N TichenorWe tested the hypothesis that the stretch-activated, four-transmembrane domain, two pore potassium channels (K2P), TREK-1 and TRAAK are gestationally-regulated in human myometrium and contribute to uterine relaxation during pregnancy until labor.We determined the gene and protein expression of K2P channels in non-pregnant, pregnant term and preterm laboring myometrium. We employed both molecular biological and functional studies of K2P channels in myometrial samples taken from women undergoing cesarean delivery of a fetus.TREK-1, but not TREK-2, channels are expressed in human myometrium and significantly up-regulated during pregnancy. Down-regulation of TREK-1 message was seen by Q-PCR in laboring tissues consistent with a role for TREK-1 in maintaining uterine quiescence prior to labor. The TRAAK channel was unregulated in the same women. Blockade of stretch-activated channels with a channel non-specific tarantula toxin (GsMTx-4) or the more specific TREK-1 antagonist L-methionine ethyl ester altered contractile frequency in a dose-dependent manner in pregnant myometrium. Arachidonic acid treatment lowered contractile tension an effect blocked by fluphenazine. Functional studies are consistent with a role for TREK-1 in uterine quiescence.We provide evidence supporting a role for TREK-1 in contributing to uterine quiescence during gestation and hypothesize that dysregulation of this mechanism may underlie certain cases of spontaneous pre-term birth.http://europepmc.org/articles/PMC2928262?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Iain L O Buxton Cherie A Singer Jennifer N Tichenor |
spellingShingle |
Iain L O Buxton Cherie A Singer Jennifer N Tichenor Expression of stretch-activated two-pore potassium channels in human myometrium in pregnancy and labor. PLoS ONE |
author_facet |
Iain L O Buxton Cherie A Singer Jennifer N Tichenor |
author_sort |
Iain L O Buxton |
title |
Expression of stretch-activated two-pore potassium channels in human myometrium in pregnancy and labor. |
title_short |
Expression of stretch-activated two-pore potassium channels in human myometrium in pregnancy and labor. |
title_full |
Expression of stretch-activated two-pore potassium channels in human myometrium in pregnancy and labor. |
title_fullStr |
Expression of stretch-activated two-pore potassium channels in human myometrium in pregnancy and labor. |
title_full_unstemmed |
Expression of stretch-activated two-pore potassium channels in human myometrium in pregnancy and labor. |
title_sort |
expression of stretch-activated two-pore potassium channels in human myometrium in pregnancy and labor. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2010-08-01 |
description |
We tested the hypothesis that the stretch-activated, four-transmembrane domain, two pore potassium channels (K2P), TREK-1 and TRAAK are gestationally-regulated in human myometrium and contribute to uterine relaxation during pregnancy until labor.We determined the gene and protein expression of K2P channels in non-pregnant, pregnant term and preterm laboring myometrium. We employed both molecular biological and functional studies of K2P channels in myometrial samples taken from women undergoing cesarean delivery of a fetus.TREK-1, but not TREK-2, channels are expressed in human myometrium and significantly up-regulated during pregnancy. Down-regulation of TREK-1 message was seen by Q-PCR in laboring tissues consistent with a role for TREK-1 in maintaining uterine quiescence prior to labor. The TRAAK channel was unregulated in the same women. Blockade of stretch-activated channels with a channel non-specific tarantula toxin (GsMTx-4) or the more specific TREK-1 antagonist L-methionine ethyl ester altered contractile frequency in a dose-dependent manner in pregnant myometrium. Arachidonic acid treatment lowered contractile tension an effect blocked by fluphenazine. Functional studies are consistent with a role for TREK-1 in uterine quiescence.We provide evidence supporting a role for TREK-1 in contributing to uterine quiescence during gestation and hypothesize that dysregulation of this mechanism may underlie certain cases of spontaneous pre-term birth. |
url |
http://europepmc.org/articles/PMC2928262?pdf=render |
work_keys_str_mv |
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