The Specific Contribution of the Novel Alpha-1D Adrenoceptor to the Contraction of Vascular Smooth Muscle

Overview

Journal J Pharmacol Exp Ther

Specialty Pharmacology

Date 1995 Dec 1

PMID 8531132

Citations 42

Authors

M T Piascik

R D Guarino

M S Smith

E E Soltis

D L Saussy Jr

D M Perez

Affiliations

Soon will be listed here.

Abstract

With a selective antagonist, the specific contribution of the alpha-1D adrenoceptor (AR) to vascular smooth muscle contraction has been assessed. BMY 7378 bound to membranes expressing the cloned rat alpha-1D AR with a > 100-fold higher affinity (K1 = 2 nM) than binding to either the cloned rat alpha-1A AR (Ki = 800 nM) or the hamster alpha-1B AR (Ki = 600 nM). BMY 7378 exhibited differential potency in inhibiting vascular smooth muscle contraction. In the rat aorta and iliac artery, BMY 7378 was a high-affinity antagonist, producing parallel shifts in the phenylephrine concentration-response curve. The dissociation constants for this compound by Schild analysis were 0.95 and 4 nM for the aorta and iliac artery, respectively. The slopes of these Schild plots were not significantly different from unity. BMY 7378 was a weak antagonist in the rat caudal, mesenteric resistance and renal arteries, with Schild slopes significantly < 1. With ribonuclease protection assays, alpha-1D mRNA was found in all blood vessels examined. These data suggest that (1) BMY 7378 is a selective alpha-1D AR antagonist that can be used in functional systems to assess the contribution of this receptor in vascular smooth muscle contraction; (2) the alpha-1D AR appears to play a major role in the contraction of the aorta and iliac artery; (3) despite the fact that the mRNA for the alpha-1D AR can be detected in the caudal, mesenteric resistance (4) and renal arteries, it does not appear to play a role in mediating contraction of these blood vessels; and (4) expression of alpha-1D mRNA in a particular artery does not ensure that this receptor is involved in regulating the contraction of that artery.

Citing Articles

Adrenoceptors: Receptors, Ligands and Their Clinical Uses, Molecular Pharmacology and Assays.

Baker J, Summers R Handb Exp Pharmacol. 2024; 285:55-145.

PMID: 38926158 DOI: 10.1007/164_2024_713.

Adrenoceptors in the Eye - Physiological and Pathophysiological Relevance.

Ruan Y, Buonfiglio F, Gericke A Handb Exp Pharmacol. 2023; 285:453-505.

PMID: 38082203 DOI: 10.1007/164_2023_702.

Role of sympathetic pathway in light-phase time-restricted feeding-induced blood pressure circadian rhythm alteration.

Hou T, Chacon A, Su W, Katsumata Y, Guo Z, Gong M Front Nutr. 2022; 9:969345.

PMID: 36159491 PMC: 9493072. DOI: 10.3389/fnut.2022.969345.

The Role of Adrenoceptors in the Retina.

Ruan Y, Bohmer T, Jiang S, Gericke A Cells. 2020; 9(12).

PMID: 33287335 PMC: 7761662. DOI: 10.3390/cells9122594.

Cardiac and Vascular α-Adrenoceptors in Congestive Heart Failure: A Systematic Review.

Kayki-Mutlu G, Papazisi O, Palmen M, Danser A, Michel M, Arioglu-Inan E Cells. 2020; 9(11).

PMID: 33158106 PMC: 7694190. DOI: 10.3390/cells9112412.