Literature DB >> 18485831

Pharmacological endothelin receptor interaction does not occur in veins from ET(B) receptor deficient rats.

Keshari Thakali1, James J Galligan, Gregory D Fink, Cheryl E Gariepy, Stephanie W Watts.   

Abstract

Heterodimerization of G-protein coupled receptors can alter receptor pharmacology. ET A and ET B receptors heterodimerize when co-expressed in heterologous expression lines. We hypothesized that ET A and ET B receptors heterodimerize and pharmacologically interact in vena cava from wild-type (WT) but not ET B receptor deficient (sl/sl) rats. Pharmacological endothelin receptor interaction was assessed by comparing ET-1-induced contraction in rings of rat thoracic aorta and thoracic vena cava from male Sprague Dawley rats under control conditions, ET A receptor blockade (atrasentan, 10 nM), ET B receptor blockade (BQ-788, 100 nM) or ET B receptor desensitization (Sarafotoxin 6c, 100 nM) and ET A plus ET B receptor blockade or ET A receptor blockade plus ET B receptor desensitization. In addition, similar pharmacological ET receptor antagonism experiments were performed in rat thoracic aorta and vena cava from WT and sl/sl rats. ET A but not ET B receptor blockade or ET B receptor desensitization inhibited aortic and venous ET-1-induced contraction. In vena cava but not aorta, when ET B receptors were blocked (BQ-788, 100 nM) or desensitized (S6c, 100 nM), atrasentan caused a greater inhibition of ET-1-induced contraction. Vena cava from WT but not sl/sl rats exhibited similar pharmacological ET receptor interaction. Immunocytochemistry was performed on freshly dissociated aortic and venous vascular smooth muscle cells to determine localization of ET A and ET B receptors. ET A and ET B receptors qualitatively co-localized more strongly to the plasma membrane of aortic compared to venous vascular smooth muscle cells. Our data suggest that pharmacological ET A and ET B receptor interaction may be dependent on the presence of functional ET B receptors and independent of receptor location.

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Year:  2008        PMID: 18485831      PMCID: PMC2529478          DOI: 10.1016/j.vph.2008.03.005

Source DB:  PubMed          Journal:  Vascul Pharmacol        ISSN: 1537-1891            Impact factor:   5.773


  30 in total

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3.  Comparison of the contractile and calcium-increasing properties of platelet-activating factor and endothelin-1 in the rat mesenteric artery and vein.

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6.  Ligand-dependent differences in the internalization of endothelin A and endothelin B receptor heterodimers.

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7.  Arteries and veins desensitize differently to endothelin.

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8.  Biochemical and pharmacological profile of a potent and selective endothelin B-receptor antagonist, BQ-788.

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Journal:  Proc Natl Acad Sci U S A       Date:  1994-05-24       Impact factor: 11.205

9.  Null mutation of endothelin receptor type B gene in spotting lethal rats causes aganglionic megacolon and white coat color.

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10.  Endothelin-1-induced venous contraction is maintained in DOCA-salt hypertension; studies with receptor agonists.

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  5 in total

1.  ET-1 induced Elevation of intracellular calcium in clonal neuronal and embryonic kidney cells involves endogenous endothelin-A receptors linked to phospholipase C through Gα(q/11).

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4.  A comparison of reactive oxygen species metabolism in the rat aorta and vena cava: focus on xanthine oxidase.

Authors:  Theodora Szasz; Janice M Thompson; Stephanie W Watts
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5.  Modification of proteins by norepinephrine is important for vascular contraction.

Authors:  Kyle B Johnson; Janice M Thompson; Stephanie W Watts
Journal:  Front Physiol       Date:  2010-10-04       Impact factor: 4.566

  5 in total

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