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AT1-receptor blockade, but not renin inhibition, reduces aneurysm growth and cardiac failure in fibulin-4 mice

Authors :
Jeroen Essers
Yanto Ridwan
Elza D. van Deel
Luuk te Riet
Els Moltzer
A.H. Jan Danser
Ingrid M. Garrelds
Paula M. van Heijningen
Bibi S. van Thiel
Jan Lukas Robertus
Richard van Veghel
Nicole van Vliet
Marcel Vermeij
Ingrid van der Pluijm
Internal Medicine
Surgery
Cardiology
Molecular Genetics
Pathology
Radiotherapy
Source :
Journal of Hypertension, 34(4), 654-665. Lippincott Williams & Wilkins
Publication Year :
2016

Abstract

textabstractAims: Increasing evidence supports a role for the angiotensin II-AT 1 -receptor axis in aneurysm development. Here, we studied whether counteracting this axis via stimulation of AT 2 receptors is beneficial. Such stimulation occurs naturally during AT 1 -receptor blockade with losartan, but not during renin inhibition with aliskiren. Methods and results: Aneurysmal homozygous fibulin-4 R/R mice, displaying a four-fold reduced fibulin-4 expression, were treated with placebo, losartan, aliskiren, or the β-blocker propranolol from day 35 to 100. Their phenotype includes cystic media degeneration, aortic regurgitation, left ventricular dilation, reduced ejection fraction, and fractional shortening. Although losartan and aliskiren reduced hemodynamic stress and increased renin similarly, only losartan increased survival. Propranolol had no effect. No drug rescued elastic fiber fragmentation in established aneurysms, although losartan did reduce aneurysm size. Losartan also increased ejection fraction, decreased LV diameter, and reduced cardiac pSmad2 signaling. None of these effects were seen with aliskiren or propranolol. Longitudinal micro-CT measurements, a novel method in which each mouse serves as its own control, revealed that losartan reduced LV growth more than aneurysm growth, presumably because the heart profits both from the local (cardiac) effects of losartan and its effects on aortic root remodeling. Conclusion: Losartan, but not aliskiren or propranolol, improved survival in fibulin-4 R/R mice. This most likely relates to its capacity to improve structure and function of both aorta and heart. The absence of this effect during aliskiren treatment, despite a similar degree of blood pressure reduction and renin-angiotensin system blockade, suggests that it might be because of AT 2 -receptor stimulation.

Details

ISSN :
02636352
Database :
OpenAIRE
Journal :
Journal of Hypertension, 34(4), 654-665. Lippincott Williams & Wilkins
Accession number :
edsair.doi.dedup.....cf5872d9eebfd9ef16cd64db29314bb7