Angiotensin AT(1B) receptor mediates calcium signaling in vascular smooth muscle cells of AT(1A) receptor-deficient mice

Zhu, Zhiming and Zhang, Sunny H. and Wagner, Charlotte and Kurtz, Armin and Maeda, Nobuyo and Coffman, Thomas and Arendshorst, William J. (1998) Angiotensin AT(1B) receptor mediates calcium signaling in vascular smooth muscle cells of AT(1A) receptor-deficient mice. HYPERTENSION, 31 (5). pp. 1171-1177. ISSN 0194-911X, 1524-4563

Full text not available from this repository. (Request a copy)

Abstract

Our studies on angiotensin II receptor subtype 1A (AT(1A)) knockout mice define how endogenous receptors other than AT(1A)receptors stimulate changes in cytosolic calcium concentration ([Ca2+](i)) in cultured aortic vascular smooth muscle cells (VSMCs). Wild-type cells have a 1.7 ratio of AT(1A)/AT(1B) receptor mRNA as determined by semiquantitative reverse transcriptase-polymerase chain reaction. Mutant cells express AT(1B) receptor mRNA but not that for the AT(1A) receptor. In wild-type cells with AT(1A) present, Ang II (10(-7) mol/L) produces a characteristic rapid peak increase in [Ca2+](i) of 150 to 180 nmol/L, followed by a plateau phase characterized by a sustained 70 to 80 nmol/L increase in [Ca2+](i). An unexpected finding was that the magnitude and time-dependent pattern of [Ca2+](i) changes produced by Ang II were similar in cells that lacked AT(1A) receptors but possessed AT(1B) receptors. The response in mutant cells indicates effective coupling of an Ang II receptor to one or more second messenger systems. The similarity of response patterns between cells with and without AT(1A) receptors suggests that non-AT(1A) receptors are functionally linked to similar signal transduction pathways in mutant cells, The fact that mutant and wild-type cells exhibit similar patterns of calcium mobilization and entry supports the notion that AT(1A) and non-AT(1A) receptors share common signal transduction pathways. The AT(2) receptor ligands PD-123319 and CGP-42112 do not alter Ang II effects in either VSMC type, suggesting a paucity of AT(2) receptors and/or an absence of their linkage to [Ca2+](i) pathways. The nonpeptide AT(1) receptor blocker losartan antagonizes Ang II-induced [Ca2+](i) increases in both cell groups, supporting mediation by native AT(1B) receptors and effective coupling of this subtype to second messenger systems leading to calcium entry and mobilization. Our results demonstrate that Ang II causes calcium signaling in AT(1A)-deficient VSMCs that is mediated by an endogenous losartan-sensitive AT(1B) receptor.

Item Type: Article
Uncontrolled Keywords: HAMSTER OVARY CELLS; II TYPE-1 RECEPTOR; DIFFERENTIAL REGULATION; GENE-EXPRESSION; BLOOD-PRESSURE; RAT; TRANSDUCTION; SUBTYPES; GROWTH; AT1A; muscle, smooth, vascular; angiotensin II; receptors, angiotensin; calcium channels; antagonists; losartan; fura 2
Subjects: 500 Science > 570 Life sciences
Divisions: Biology, Preclinical Medicine > Institut für Physiologie > Prof. Dr. Armin Kurtz
Depositing User: Dr. Gernot Deinzer
Date Deposited: 23 May 2023 13:06
Last Modified: 23 May 2023 13:06
URI: https://pred.uni-regensburg.de/id/eprint/49841

Actions (login required)

View Item View Item
pred is powered by EPrints 3.4 which is developed by the School of Electronics and Computer Science at the University of Southampton. More information and software credits.