Regulation of the Ca super(2+)-sensitive Domains of the Maxi-K Channel in the Mouse Myometrium during Gestation

Regulation of the Ca super(2+)-sensitive Domains of the Maxi-K Channel in the Mouse Myometrium during Gestation

Large conductance Ca super(2+)-activated K super(+) channels (maxi-K channels) are known to modulate uterine activity during gestation. Electrophysiological recordings demonstrate that myometrial maxi-K current is suppressed in term-pregnant compared to non-pregnant mice. We sought to determine whet...

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Veröffentlicht in:The Journal of biological chemistry 2000-09, Vol.275 (36), p.27712-27719
Hauptverfasser: Benkusky, NA, Fergus, D J, Zucchero, T M, England, S K
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myometrium
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creator Benkusky, NA
Fergus, D J
Zucchero, T M
England, S K
description Large conductance Ca super(2+)-activated K super(+) channels (maxi-K channels) are known to modulate uterine activity during gestation. Electrophysiological recordings demonstrate that myometrial maxi-K current is suppressed in term-pregnant compared to non-pregnant mice. We sought to determine whether maxi-K current suppression is due to reduction of maxi-K channel protein or differential expression of maxi-K channel isoforms that vary in their Ca super(2+) and voltage sensitivities. Immunoblot analyses show an increase of maxi-K channel protein throughout gestation. Polymerase chain reaction of mouse myometrial cDNA identified four alternatively spliced sites within the maxi-K transcript and three within the Ca super(2+)-sensitive "tail" domain. Ribonuclease protection analyses demonstrate that total channel transcript levels mimic protein expression; however transcript levels of alternatively spliced regions of regulatory domains that alter sensitivity to voltage and Ca super(2+) differ in their gestational expression. An insert that increases the maxi-K channel sensitivity to voltage and Ca super(2+) is present at steady levels throughout gestation, differing from total channel transcript regulation. The insert-less form of this transcript, which reduces the channel voltage and Ca super(2+) sensitivity, is not detected until midterm pregnancy. These findings verify that multiple isoforms of the maxi-K channel are present in the mouse myometrium and are regulated differentially during gestation, which is a likely mechanism for modulation of myometrial excitability during pregnancy.
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title Regulation of the Ca super(2+)-sensitive Domains of the Maxi-K Channel in the Mouse Myometrium during Gestation
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