The β-arrestin-biased ligand TRV120023 inhibits angiotensin II-induced cardiac hypertrophy while preserving enhanced myofilament response to calcium

Michelle M Monasky; Domenico M Taglieri; Marcus Henze; Chad M Warren; Megan S Utter; David G Soergel; Jonathan D Violin; R John Solaro

doi:10.1152/ajpheart.00327.2013

The β-arrestin-biased ligand TRV120023 inhibits angiotensin II-induced cardiac hypertrophy while preserving enhanced myofilament response to calcium

Am J Physiol Heart Circ Physiol. 2013 Sep 15;305(6):H856-66. doi: 10.1152/ajpheart.00327.2013. Epub 2013 Jul 19.

Authors

Michelle M Monasky¹, Domenico M Taglieri, Marcus Henze, Chad M Warren, Megan S Utter, David G Soergel, Jonathan D Violin, R John Solaro

Affiliation

¹ Department of Physiology and Biophysics and Center for Cardiovascular Research, College of Medicine, University of Illinois, Chicago, Illinois; and.

Abstract

In the present study, we compared the cardioprotective effects of TRV120023, a novel angiotensin II (ANG II) type 1 receptor (AT1R) ligand, which blocks G protein coupling but stimulates β-arrestin signaling, against treatment with losartan, a conventional AT1R blocker in the treatment of cardiac hypertrophy and regulation of myofilament activity and phosphorylation. Rats were subjected to 3 wk of treatment with saline, ANG II, ANG II + losartan, ANG II + TRV120023, or TRV120023 alone. ANG II induced increased left ventricular mass compared with rats that received ANG II + losartan or ANG II + TRV120023. Compared with saline controls, ANG II induced a significant increase in pCa50 and maximum Ca(2+)-activated myofilament tension but reduced the Hill coefficient (nH). TRV120023 increased maximum tension and pCa50, although to lesser extent than ANG II. In contrast to ANG II, TRV120023 increased nH. Losartan blocked the effects of ANG II on pCa50 and nH and reduced maximum tension below that of saline controls. ANG II + TRV120023 showed responses similar to those of TRV120023 alone; compared with ANG II + losartan, ANG II + TRV120023 preserved maximum tension and increased both pCa50 and cooperativity. Tropomyosin phosphorylation was lower in myofilaments from saline-treated hearts compared with the other groups. Phosphorylation of cardiac troponin I was significantly reduced in ANG II + TRV120023 and TRV120023 groups versus saline controls, and myosin-binding protein C phosphorylation at Ser(282) was unaffected by ANG II or losartan but significantly reduced with TRV120023 treatment compared with all other groups. Our data indicate that TRV120023-related promotion of β-arrestin signaling and enhanced contractility involves a mechanism promoting the myofilament response to Ca(2+) via altered protein phosphorylation. Selective activation of β-arrestin-dependent pathways may provide advantages over conventional AT1R blockers.

Keywords: angiotensin; angiotensin II type 1 receptor; hypertrophy; myofilament calcium sensitivity; β-arrestin.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Angiotensin II
Animals
Arrestins / metabolism*
Calcium / metabolism*
Cardiomegaly / chemically induced
Cardiomegaly / drug therapy*
Cardiomegaly / physiopathology*
Cardiotonic Agents / administration & dosage
Heart Ventricles / drug effects
Heart Ventricles / pathology
Heart Ventricles / physiopathology*
Male
Myocardial Contraction / drug effects
Myofibrils / drug effects*
Oligopeptides / administration & dosage*
Organ Size / drug effects
Rats
Rats, Sprague-Dawley
Treatment Outcome
Up-Regulation / drug effects
beta-Arrestins

Substances

Arrestins
Cardiotonic Agents
Oligopeptides
beta-Arrestins
sarcosine-arginyl-valyl-tyrosyl-lysyl-histidyl-prolyl-alanine
Angiotensin II
Calcium

Abstract

Publication types

MeSH terms

Substances

Grants and funding