학술논문
MicroRNA-155 Amplifies Nitric Oxide/cGMP Signaling and Impairs Vascular Angiotensin II Reactivity in Septic Shock
Document Type
Academic Journal
Author
Vasques-Nóvoa, Francisco; Laundos, Tiago L.; Cerqueira, Rui J.; Quina-Rodrigues, Catarina; Soares-dos-Reis, Ricardo; Baganha, Fabiana; Ribeiro, Sara; Mendonça, Luís; Gonçalves, Francisco; Reguenga, Carlos; Verhesen, Wouter; Carneiro, Fátima; Paiva, José Artur; Schroen, Blanche; Castro-Chaves, Paulo; Pinto-do-Ó, Perpétua; Nascimento, Diana S.; Heymans, Stephane; Leite-Moreira, Adelino F.; Roncon-Albuquerque, Roberto, Jr
Source
Critical Care Medicine. Sep 01, 2018 46(9):e945-e954
Subject
Language
English
ISSN
0090-3493
Abstract
OBJECTIVES:: Septic shock is a life-threatening clinical situation associated with acute myocardial and vascular dysfunction, whose pathophysiology is still poorly understood. Herein, we investigated microRNA-155–dependent mechanisms of myocardial and vascular dysfunction in septic shock. DESIGN:: Prospective, randomized controlled experimental murine study and clinical cohort analysis. SETTING:: University research laboratory and ICU at a tertiary-care center. PATIENTS:: Septic patients, ICU controls, and healthy controls. Postmortem myocardial samples from septic and nonseptic patients. Ex vivo evaluation of arterial rings from patients undergoing coronary artery bypass grafting. SUBJECTS:: C57Bl/6J and genetic background–matched microRNA-155 knockout mice. INTERVENTIONS:: Two mouse models of septic shock were used. Genetic deletion and pharmacologic inhibition of microRNA-155 were performed. Ex vivo myographic studies were performed using mouse and human arterial rings. MEASUREMENTS AND MAIN RESULTS:: We identified microRNA-155 as a highly up-regulated multifunctional mediator of sepsis-associated cardiovascular dysfunction. In humans, plasma and myocardial microRNA-155 levels correlate with sepsis-related mortality and cardiac injury, respectively, whereas in murine models, microRNA-155 deletion and pharmacologic inhibition attenuate sepsis-associated cardiovascular dysfunction and mortality. MicroRNA-155 up-regulation in septic myocardium was found to be mostly supported by microvascular endothelial cells. This promoted myocardial microvascular permeability and edema, bioenergetic deterioration, contractile dysfunction, proinflammatory, and nitric oxide-cGMP-protein kinase G signaling overactivation. In isolate cardiac microvascular endothelial cells, microRNA-155 up-regulation significantly contributes to LPS-induced proinflammatory cytokine up-regulation, leukocyte adhesion, and nitric oxide overproduction. Furthermore, we identified direct targeting of CD47 by microRNA-155 as a novel mechanism of myocardial and vascular contractile depression in sepsis, promoting microvascular endothelial cell and vascular insensitivity to thrombospondin-1–mediated inhibition of nitric oxide production and nitric oxide–mediated vasorelaxation, respectively. Additionally, microRNA-155 directly targets angiotensin type 1 receptor, decreasing vascular angiotensin II reactivity. Deletion of microRNA-155 restored angiotensin II and thrombospondin-1 vascular reactivity in LPS-exposed arterial rings. CONCLUSIONS:: Our study demonstrates multiple new microRNA-155–mediated mechanisms of sepsis-associated cardiovascular dysfunction, supporting the translational potential of microRNA-155 inhibition in human septic shock.