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Important pathophysiologic mechanisms in HF (1). Important pathophysiologic mechanisms in HF (2). Important pathophysiologic mechanisms in HF (3). Neurohormonal model of HF. -Blockade normalizes Ang II-provoked release of norepinephrine in HF. Molecular model of HF.
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-Blockade normalizes Ang II-provoked release of norepinephrine in HF
Regulation of key molecules in cardiac EC coupling bystress-activated pathways
Myocardial force generation increases in response to -blockade in HF after exposure to isoproterenol
The RAAS in HF Angiotensinogen Kininogens Angiotensin I Bradykinin Nonspecific chymases ACE/kininase II • Bradykinin receptor • Norepinephrine • Vasodilation • Vessel permeability • tPA/prostaglandin release ACEinhibitors Angiotensin II Inactive peptides ARB • AT1 receptor • Myocardial fibrosis • Norepinephrine • Vasoconstriction • PAI/endothelin AT2 receptor Myocardial fibrosis Adrenal catechols ? Apoptosis Sympatheticactivity Nitric oxide Aldosterone Aldosteroneantagonists Improvedendothelial function Increased afterload disease progression The RAAS in HF RAAS = renin-angiotensin-aldosterone system Jamali AH et al. Arch Intern Med. 2001;161:667-72.
RESOLVD: Ang II concentrations similar at baseline and study end
AT1-receptor blockade improves vasorelaxation in HF by upregulation of eNOS via AT2 receptors
