Identification and characterization of alamandine-(1-5), a new component of the Renin-Angiotensin System with unique properties

  1. Melissa Tainan Silva Dias
  2. Sthefanie Chaves de Almeida Gonçalves
  3. Filipe Alex da Silva
  4. Lucas Rodrigues-Ribeiro
  5. Kamylle Silva Ferraz
  6. Sérgio Scalzo
  7. Matheus F. Itaborahy
  8. Nícia Pedreira Soares
  9. Danilo Augusto Alves Pereira
  10. Pedro Alves Soares
  11. João Batista Rodrigues Dutra
  12. Carolina Fonseca de Barros
  13. Uri Flegler Vieira-Machado
  14. Isadora Zhong Liang Ferreira Feng
  15. Ana Caroline Ventris de Godoy
  16. Adelson Héric Alves Monteiro
  17. Marcos Eliezeck
  18. Bruno Sanches
  19. André Monteiro
  20. Amanda de Sá Martins de Bessa
  21. Ana Paula Davel
  22. Natália Nóbrega
  23. Júlia Rezende Ribeiro
  24. Maria Luiza Dias-Pinto
  25. Bruno Durante da Silva
  26. Leandro Eziquiel de Souza
  27. Amanda de A. Silva
  28. Michael Bader
  29. Natália Alenina
  30. Luciano dos Santos Aggum Capettini
  31. Maria José Campagnole-Santos
  32. Thiago Verano-Braga
  33. Marco Antônio Peliky Fontes
  34. Andrea Siqueira Haibara
  35. Daniel Campos Vilella
  36. Maria Claudia Irigoyen
  37. Fernanda Ribeiro Marins
  38. Carlos Henrique de Castro
  39. Ana Cristina Simões-e-Silva
  40. Maria de Fátima Leite
  41. Silvia Guatimosim
  42. Robson A. S. Santos
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Abstract

The renin-angiotensin system (RAS) comprises a biochemical cascade that hydrolyzes angiotensinogen into several different bioactive peptides, which can activate different receptors promoting plenty of specific effects. The aim of this study was to evaluate the presence of the putative product of alamandine, the pentapeptide alamandine-(1-5) in the circulation and its biological activity. To accomplish this we have used mass spectrometry (MALDI/TOF/TOF, LC-MS/MS) and several methodologies including isolated blood vessels, isolated perfused hearts, isolated cardiomyocytes, blood pressure recording in freely-moving normotensive and hypertensive rats (SHR), high resolution echocardiography (VEVO 2100), central administration (ICV infusion and microinjection in the insular cortex), cell culture (endothelial cells and GPCR-transfected CHO cells) and wild type and Mas, MrgD or AT2R deficient mice. Our results show that alamandine-(1-5) circulates in the human and rodent blood and promotes many biological central and peripheral actions. More importantly, its plasma concentration is increased in pediatric nephropathic patients. A major role for plasma ACE activity in the formation of alamandine-(1-5) from alamandine was observed using plasma samples from Angiotensinogen-KO mice. Alamandine-(1-5) increased Baroreflex sensitivity and produced a long-lasting (∼6 hours) anti-hypertensive effect in SHR, associated with a significant reduction in cardiac output. A particularly important effect of this pentapeptide was observed in isolated perfused heart and cardiomyocyte contractility (reduced inotropism). It was capable of stimulating NO production through all receptors from the renin-angiotensin protective arm, (MAS, MrgD and AT2R) in CHO-transfected cells. Our data shows that Alamandine-(1-5) exhibits selective actions that set it apart from traditional concepts of the vasodilatory axis of the RAS and that are possibly intricately linked to a complex interplay between Mas, MrgD and AT2 receptors. This novel finding suggests that RAS may possess a complexity that surpasses our current understanding.

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  1. Version published to 10.1101/2024.04.27.591083v1 on bioRxiv