Literature DB >> 18854423

Both TASK-3 and TREK-1 two-pore loop K channels are expressed in H295R cells and modulate their membrane potential and aldosterone secretion.

Tanja Brenner1, Kevin M O'Shaughnessy.   

Abstract

The rate of aldosterone synthesis by adrenal glomerulosa cells relies on the selective permeability of the glomerulosa cell to K(+) ions. In rodent and bovine adrenal glomerulosa cells, this background potassium current is provided by a two-pore loop potassium (K2P) channel: largely TASK-3 in the rat and TREK-1 in the cow. The nature of the K2P channel in the human adrenal cortex is not known, and we have addressed this issue here using the H295R human adrenal cell line. We show that these cells express mRNA and protein for both TASK-3 and TREK-1 K2P channels. Using a potentiometric dye (FMP), we also show that TASK-3 and TREK-1 channel modulators can affect the membrane potential of H295R cells. Transfecting H295R cells with TASK-3 or TREK-1 dominant-negative mutants (TASK-3 G95E or TREK-1 G144E) produced depolarization of H295R cells and altered K-stimulated aldosterone secretion. Finally, transfection of a constitutively active mutant of Galpha(q) into H295R cells (GTPase-deficient Galpha(q)-QL) depolarized them and increased basal aldosterone secretion. Taken together, our data support both TASK-3 and TREK-1 as being functionally operational in the H295R cell line. This suggests that human adrenal glomerulosa cells may utilize both of these K2P channels for their background potassium current.

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Year:  2008        PMID: 18854423     DOI: 10.1152/ajpendo.90652.2008

Source DB:  PubMed          Journal:  Am J Physiol Endocrinol Metab        ISSN: 0193-1849            Impact factor:   4.310


  13 in total

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2.  Calcium-dependent inhibition of adrenal TREK-1 channels by angiotensin II and ionomycin.

Authors:  John J Enyeart; Haiyan Liu; Judith A Enyeart
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Review 3.  Genetics of hypertension and cardiovascular disease and their interconnected pathways: lessons from large studies.

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Review 4.  Molecular regulations governing TREK and TRAAK channel functions.

Authors:  Jacques Noël; Guillaume Sandoz; Florian Lesage
Journal:  Channels (Austin)       Date:  2011-09-01       Impact factor: 2.581

5.  Dominant negative effects of a non-conducting TREK1 splice variant expressed in brain.

Authors:  Emma L Veale; Kathryn A Rees; Alistair Mathie; Stefan Trapp
Journal:  J Biol Chem       Date:  2010-07-06       Impact factor: 5.157

Review 6.  Minireview: potassium channels and aldosterone dysregulation: is primary aldosteronism a potassium channelopathy?

Authors:  Celso E Gomez-Sanchez; Kenji Oki
Journal:  Endocrinology       Date:  2013-12-20       Impact factor: 4.736

Review 7.  Two-pore domain potassium channels in the adrenal cortex.

Authors:  Sascha Bandulik; Philipp Tauber; Enzo Lalli; Jacques Barhanin; Richard Warth
Journal:  Pflugers Arch       Date:  2014-10-23       Impact factor: 3.657

8.  Novel Insertion Mutation in KCNJ5 Channel Produces Constitutive Aldosterone Release From H295R Cells.

Authors:  Iris Hardege; Shengxin Xu; Richard D Gordon; Andrew J Thompson; Nichola Figg; Michael Stowasser; Ruth Murrell-Lagnado; Kevin M O'Shaughnessy
Journal:  Mol Endocrinol       Date:  2015-09-04

9.  TASK-1 Regulates Apoptosis and Proliferation in a Subset of Non-Small Cell Lung Cancers.

Authors:  Katharina Leithner; Birgit Hirschmugl; Yingji Li; Bi Tang; Rita Papp; Chandran Nagaraj; Elvira Stacher; Philipp Stiegler; Jörg Lindenmann; Andrea Olschewski; Horst Olschewski; Andelko Hrzenjak
Journal:  PLoS One       Date:  2016-06-13       Impact factor: 3.240

Review 10.  Ion Channel Function and Electrical Excitability in the Zona Glomerulosa: A Network Perspective on Aldosterone Regulation.

Authors:  Paula Q Barrett; Nick A Guagliardo; Douglas A Bayliss
Journal:  Annu Rev Physiol       Date:  2020-11-11       Impact factor: 19.318

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