Angiotensin-(1-7) improves oxygenation, while reducing cellular infiltrate and fibrosis in experimental Acute Respiratory Distress Syndrome

Zambelli, Vanessa; Bellani, Giacomo; Borsa, R.; Pozzi, Federico; Grassi, Alice; Scanziani, Margherita; Castiglioni, Valentina; Masson, Serge; Decio, Alessandra; Laffey, John G.; Latini, Roberto; Pesenti, Antonio

doi:10.1186/s40635-015-0044-3

Cited by 91 publications

(96 citation statements)

References 44 publications

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“…In this model of ALI, all tested TWs for Ang‐(1–7) showed some form of therapeutic benefit, in that they alleviated OA‐induced increases in permeability, inflammatory markers or haemodynamic alterations. This finding is in line with prior work in which we and others have recently demonstrated the therapeutic potential of Ang‐(1–7) for the treatment of experimental ALI (Klein et al , ; Li et al , ; Zambelli et al , ). Of the four different time windows tested, the best protection in terms of lung vascular barrier function, inflammatory and haemodynamic parameters was provided by a continuous infusion of Ang‐(1–7) starting at the time of injury and continuing until the end of the experimental period (TW2).…”

Section: Discussionmentioning

confidence: 99%

“…However, metabolism of AngII by ACE2 concomitantly leads to the generation of Ang‐(1–7), which counteracts many of the effects of the AngII‐AT 1 receptor axis by signalling through its own receptor, Mas. In previous work, we and others have provided experimental proof‐of‐principle demonstrating not only that exogenous Ang‐(1–7) exerts similar or even more pronounced protective effects as recombinant ACE2 or pharmacological blockade of AT 1 receptors respectively (Klein et al , ; Li et al , ; Zambelli et al , ), but also that the protective effect of AT 1 receptor blockade is largely attributable to an enhanced signalling via the Ang‐(1–7)/Mas axis (Klein et al , ). The cellular mechanisms underlying the protective effects of Ang‐(1–7) in ALI are still incompletely understood but are likely to involve endothelial barrier‐stabilizing effects via cGMP‐dependent and cAMP‐dependent pathways, given that inhibition of NO synthase by L‐NAME inhibited the barrier‐protective effect of Ang‐(1–7) in lung microvascular endothelial cells challenged by thrombin (Klein et al , ) and that Ang‐(1–7) increased intracellular cAMP levels (Liu et al , ), which can attenuate endothelial leak (Moore et al , ) and reduce inflammatory cell infiltration (Derian et al , ).…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, we recently reported proof of principle for a highly effective therapeutic effect of Ang‐(1–7) in different preclinical models of ALI/ARDS including the model of oleic acid (OA)‐induced ALI in rats, and models of overventilation‐induced and acid instillation‐induced lung injury in mice (Klein et al , ). Meanwhile, these beneficial effects have been successfully reproduced by others, demonstrating the validity and reproducibility of this therapeutic effect in different models and laboratories respectively (Li et al , ; Zambelli et al , ). As the heptapeptide Ang‐(1–7) has already been approved by the Food and Drug http://www.oxforddictionaries.com/us/definition/english/administration#administration__11 for use in a series of clinical trials (Balingit et al , ; Pham et al , ), testing of this peptide as a therapeutic strategy for the treatment of ARDS is becoming a realistic and promising scenario.…”

Section: Introductionmentioning

confidence: 99%

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Therapeutic time window for angiotensin‐(1–7) in acute lung injury

Supé

Kohse

Gembardt

et al. 2016

British J Pharmacology

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There is presently no proven pharmacological therapy for the acute respiratory distress syndrome. Recently, we and others discovered that the heptapeptide angiotensin-(1-7) [Ang-(1-7)] shows significant beneficial effects in preclinical models of acute lung injury (ALI). Here, we aimed to identify the best time window for Ang-(1-7) administration to protect rats from oleic acid (OA) induced ALI. EXPERIMENTAL APPROACHThe effects of i.v. infused Ang-(1-7) were examined over four different time windows before or after induction of ALI in male Sprague-Dawley rats. Haemodynamic effects were continuously monitored, and loss of barrier function, inflammation and lung peptidase activities were measured as experimental endpoints. KEY RESULTSAng-(1-7) infusion provided the best protection against experimental ALI when administered by continuous infusion starting immediately after 30 min OA infusion till the end of the experiment (30-240 min). Both pretreatment (À60 to 0 min before OA) and short-term therapy (30-90 min) also had beneficial effects although less pronounced than the effects achieved with the optimal therapy window. Starting infusion of Ang-(1-7) 60 min after the end of OA treatment (90-240 min) did not protect barrier function or haemodynamics but still reduced myeloperoxidase activity and increased ACE2/ACE activity ratio respectively. CONCLUSIONS AND IMPLICATIONSOur findings indicate that early initiation of therapy after ALI and continuous drug delivery are most beneficial for optimal therapeutic efficiency of Ang-(1-7) treatment in experimental ALI and, presumably accordingly, in clinical acute respiratory distress syndrome. AbbreviationsALI, acute lung injury; Ang-(1-7), angiotensin-(1-7); AP, arterial blood pressure; ARDS, acute respiratory distress syndrome;

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Therapeutic time window for angiotensin‐(1–7) in acute lung injury

Supé

Kohse

Gembardt

et al. 2016

British J Pharmacology

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“…74,86,87 Ang (1-7) infusion in murine experimental ARDS decreased the proinflammatory response, improved lung injury scores and lung function, and decreased cellular infiltrate in piglets with acid aspiration. 74,82 These beneficial effects are mediated by downregulation of the intracellular proinflammatory NFkB cascade and increased NO synthesis. 51 A randomized controlled trial of recombinant human ACE2 in humans with ARDS showed it decreased Ang II levels and proinflammatory mediators, and augmented plasmatic surfactant protein D, with no hemodynamic side effects.…”

Section: Angiotensin-converting Enzymes In Acute Respiratory Distressmentioning

confidence: 93%

“…73 In sheer contrast, activation of the Ang (1-7)/ACE2 axis inhibits ROS production, downregulates proinflammatory cytokine secretion, and has immunomodulatory tissue-protective features (see Box 2). 60,62,66,74…”

Section: Renin-angiotensin Systems and The Immune Systemmentioning

confidence: 99%

Classic and Nonclassic Renin-Angiotensin Systems in the Critically Ill

Bitker

Burrell

2019

Critical Care Clinics

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KEYWORDSAcute kidney injury Acute respiratory distress syndrome Angiotensin Angiotensin-converting enzyme Sepsis Inflammation Septic shock Renin KEY POINTSActivation of the endocrine renin-angiotensin system (RAS) cascade induces immediate metabolic, hemodynamic, and renal responses, in response to changes in blood pressure and homeostasis. Renin and angiotensin II are upregulated in the setting of sepsis and septic shock. Higher renin and angiotensin II and lower circulating angiotensin-converting enzyme levels are associated with worse survival. Classic and nonclassic RASs modulate the inflammatory and immune responses. The angiotensin II axis stimulates a proinflammatory beneficial antibacterial response. In patients with vasoplegic shock, the infusion of exogenous angiotensin II lowers vasopressor requirements, and improves renal-related outcomes. Experimental evidence supports the direct role of classic RAS in the pathophysiology of acute respiratory distress syndrome, whereas clinical data suggest a lung protective effect of angiotensin-converting enzyme 2 administration.

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RAAS Blockade and COVID‐19: Mechanistic Modeling of Mas and AT1 Receptor Occupancy as Indicators of Pro‐Inflammatory and Anti‐Inflammatory Balance

Hallow

Dave

2021

Clin Pharma and Therapeutics

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ACE inhibitors (ACEis) and angiotensin receptor blockers (ARBs) are standard-of-care treatments for hypertension and diabetes, common comorbidities among hospitalized patients with coronavirus disease 2019 (COVID-19). Their use in the setting of COVID-19 has been heavily debated due to potential interactions with ACE2, an enzyme that links the pro-inflammatory and anti-inflammatory arms of the renin angiotensin system, but also the entryway by which severe acute respiratory syndrome-coronavirus 2 (SARS-CoV-2) invades cells. ACE2 expression is altered by age, hypertension, diabetes, and the virus itself. This study integrated available information about the renin angiotensin aldosterone system (RAAS) and effects of SARS-CoV-2 and its comorbidities on ACE2 into a mechanistic mathematical model and aimed to quantitatively predict effects of ACEi/ARBs on the RAAS pro-inflammatory/ anti-inflammatory balance. RAAS blockade prior to SARS-CoV-2 infection is predicted to increase the mas-AT1 receptor occupancy ratio up to 20-fold, indicating that in patients already taking an ACEi/ARB before infection, the anti-inflammatory arm is already elevated while the pro-inflammatory arm is suppressed. Predicted proinflammatory shifts in the mas-AT1 ratio due to ACE2 downregulation by SARS-CoV-2 were small relative to antiinflammatory shifts induced by ACEi/ARB. Predicted effects of changes in ACE2 expression with comorbidities of diabetes, hypertension, or aging on mas-AT1 occupancy ratio were also relatively small. Last, predicted changes in the angiotensin (Ang(1-7)) production rate with ACEi/ARB therapy, comorbidities, or infection were all small relative to exogenous Ang(1-7) infusion rates shown experimentally to protect against acute lung injury, suggesting that any changes in the ACE2-Ang(1-7)-mas arm may not be large enough to play a major role in COVID-19 pathophysiology. Hypertension and diabetes are common comorbidities among hospitalized patients with coronavirus disease 2019 (COVID-19). 1 ACE inhibitors (ACEis) and angiotensin receptor blockers (ARBs) are standard of care treatment for these comorbidities, because they reduce cardiovascular events, kidney injury, and other vascular complications of these diseases. 2,3 There has been a good deal of

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Angiotensin-(1-7) improves oxygenation, while reducing cellular infiltrate and fibrosis in experimental Acute Respiratory Distress Syndrome

Cited by 91 publications

References 44 publications

Therapeutic time window for angiotensin‐(1–7) in acute lung injury

Therapeutic time window for angiotensin‐(1–7) in acute lung injury

Classic and Nonclassic Renin-Angiotensin Systems in the Critically Ill

RAAS Blockade and COVID‐19: Mechanistic Modeling of Mas and AT1 Receptor Occupancy as Indicators of Pro‐Inflammatory and Anti‐Inflammatory Balance

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