Is angiotensin-(3–4) (Val-Tyr), the shortest angiotensin II-derived peptide, opening new vistas on the renin–angiotensin system?

Author:

Dias Juliana123,Axelband Flavia1,Lara Lucienne S.34,Muzi-Filho Humberto23,Vieyra Adalberto235

Affiliation:

1. National Institute of Cancer, Rio de Janeiro, Brazil

2. Carlos Chagas Institute of Biophysics, Federal University of Rio de Janeiro, Brazil

3. National Center of Structural Biology and Bioimaging, Federal University of Rio de Janeiro, Brazil

4. Institute of Biomedical Sciences, Federal University of Rio de Janeiro, Brazil

5. Translational Biomedicine Graduate Program, Grande Rio University, Brazil

Abstract

Angiotensin-(3−4) (Ang-(3−4) or Val-Tyr) is the shorter angiotensin (Ang) II-derived peptide, formed through successive hydrolysis that culminates with the release of Val-Tyr as a dipeptide. It is formed both in plasma and in kidney from Ang II and Ang III, and can be considered a component of the systemic and organ-based renin–angiotensin system. It is potently antihypertensive in humans and rats, and its concerted actions on proximal tubule cells culminate in the inhibition of fluid reabsorption, hyperosmotic urinary excretion of Na+. At the renal cell signaling level, Ang-(3−4) counteracts Ang II-type 1 receptor-mediated responses by acting as an allosteric enhancer in Ang II-type 2 receptor populations that target adenosine triphosphate-dependent Ca2+ and Na+ transporters through a cyclic adenosine monophosphate-activated protein kinase pathway.

Publisher

Hindawi Limited

Subject

Endocrinology,Internal Medicine

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