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The cooperative roles of the dopamine receptors, D(1)R and D(5)R, on the regulation of renal sodium transport

Determining the individual roles of the two dopamine D(1)-like receptors (D(1)R and D(5)R) on sodium transport in the human renal proximal tubule has been complicated by their structural and functional similarity. Here we used a novel D(5)R-selective antagonist (LE-PM436) and D(1)R or D(5)R-specific...

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Autores principales: Gildea, John J., Shah, Ishan T., Van Sciver, Robert, Israel, Jonathan A., Enzensperger, Christoph, McGrath, Helen E., Jose, Pedro A., Felder, Robin A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4077925/
https://www.ncbi.nlm.nih.gov/pubmed/24552847
http://dx.doi.org/10.1038/ki.2014.5
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author Gildea, John J.
Shah, Ishan T.
Van Sciver, Robert
Israel, Jonathan A.
Enzensperger, Christoph
McGrath, Helen E.
Jose, Pedro A.
Felder, Robin A.
author_facet Gildea, John J.
Shah, Ishan T.
Van Sciver, Robert
Israel, Jonathan A.
Enzensperger, Christoph
McGrath, Helen E.
Jose, Pedro A.
Felder, Robin A.
author_sort Gildea, John J.
collection PubMed
description Determining the individual roles of the two dopamine D(1)-like receptors (D(1)R and D(5)R) on sodium transport in the human renal proximal tubule has been complicated by their structural and functional similarity. Here we used a novel D(5)R-selective antagonist (LE-PM436) and D(1)R or D(5)R-specific gene silencing to determine second messenger coupling pathways and heterologous receptor interaction between the two receptors. D(1)R and D(5)R co-localized in renal proximal tubule cells and physically interact, as determined by co-immunoprecipitation and FRET microscopy. Stimulation of renal proximal tubule cells with fenoldopam (D(1)R/D(5)R agonist) led to both adenylyl cyclase and phospholipase C (PLC) activation using real-time FRET biosensors ICUE3 and CYPHR, respectively. Fenoldopam increased cAMP accumulation and PLC activity and inhibited both NHE3 and NaKATPase activities. LE-PM436 and D(5)R siRNA blocked the fenoldopam-stimulated PLC pathway but not cAMP accumulation, while D(1)R siRNA blocked both fenoldopam-stimulated cAMP accumulation and PLC signaling. Either D(1)R or D(5)R siRNA, or LE-PM436 blocked the fenoldopam dependent inhibition of sodium transport. Further studies using the cAMP-selective D(1)R/D(5)R agonist SKF83822 and PLC-selective D(1)R/D(5)R agonist SKF83959 confirmed the cooperative influence of the two pathways on sodium transport. Thus, D(1)R and D(5)R interact in the inhibition of NHE3 and NaKATPase activity, the D(1)R primarily by cAMP, while the D(1)R/D(5)R heteromer modulates the D(1)R effect through a PLC pathway.
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spelling pubmed-40779252015-01-01 The cooperative roles of the dopamine receptors, D(1)R and D(5)R, on the regulation of renal sodium transport Gildea, John J. Shah, Ishan T. Van Sciver, Robert Israel, Jonathan A. Enzensperger, Christoph McGrath, Helen E. Jose, Pedro A. Felder, Robin A. Kidney Int Article Determining the individual roles of the two dopamine D(1)-like receptors (D(1)R and D(5)R) on sodium transport in the human renal proximal tubule has been complicated by their structural and functional similarity. Here we used a novel D(5)R-selective antagonist (LE-PM436) and D(1)R or D(5)R-specific gene silencing to determine second messenger coupling pathways and heterologous receptor interaction between the two receptors. D(1)R and D(5)R co-localized in renal proximal tubule cells and physically interact, as determined by co-immunoprecipitation and FRET microscopy. Stimulation of renal proximal tubule cells with fenoldopam (D(1)R/D(5)R agonist) led to both adenylyl cyclase and phospholipase C (PLC) activation using real-time FRET biosensors ICUE3 and CYPHR, respectively. Fenoldopam increased cAMP accumulation and PLC activity and inhibited both NHE3 and NaKATPase activities. LE-PM436 and D(5)R siRNA blocked the fenoldopam-stimulated PLC pathway but not cAMP accumulation, while D(1)R siRNA blocked both fenoldopam-stimulated cAMP accumulation and PLC signaling. Either D(1)R or D(5)R siRNA, or LE-PM436 blocked the fenoldopam dependent inhibition of sodium transport. Further studies using the cAMP-selective D(1)R/D(5)R agonist SKF83822 and PLC-selective D(1)R/D(5)R agonist SKF83959 confirmed the cooperative influence of the two pathways on sodium transport. Thus, D(1)R and D(5)R interact in the inhibition of NHE3 and NaKATPase activity, the D(1)R primarily by cAMP, while the D(1)R/D(5)R heteromer modulates the D(1)R effect through a PLC pathway. 2014-02-19 2014-07 /pmc/articles/PMC4077925/ /pubmed/24552847 http://dx.doi.org/10.1038/ki.2014.5 Text en http://www.nature.com/authors/editorial_policies/license.html#terms Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Gildea, John J.
Shah, Ishan T.
Van Sciver, Robert
Israel, Jonathan A.
Enzensperger, Christoph
McGrath, Helen E.
Jose, Pedro A.
Felder, Robin A.
The cooperative roles of the dopamine receptors, D(1)R and D(5)R, on the regulation of renal sodium transport
title The cooperative roles of the dopamine receptors, D(1)R and D(5)R, on the regulation of renal sodium transport
title_full The cooperative roles of the dopamine receptors, D(1)R and D(5)R, on the regulation of renal sodium transport
title_fullStr The cooperative roles of the dopamine receptors, D(1)R and D(5)R, on the regulation of renal sodium transport
title_full_unstemmed The cooperative roles of the dopamine receptors, D(1)R and D(5)R, on the regulation of renal sodium transport
title_short The cooperative roles of the dopamine receptors, D(1)R and D(5)R, on the regulation of renal sodium transport
title_sort cooperative roles of the dopamine receptors, d(1)r and d(5)r, on the regulation of renal sodium transport
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4077925/
https://www.ncbi.nlm.nih.gov/pubmed/24552847
http://dx.doi.org/10.1038/ki.2014.5
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