Your search keyword '"Mas receptor"' showing total 11 results

1. Endotoxin-induced skeletal muscle wasting is prevented by angiotensin-(1-7) through a p38 MAPK-dependent mechanism.

Author

Morales, María Gabriela, Olguín, Hugo, Di Capua, Gabriella, Brandan, Enrique, Simon, Felipe, and Cabello-Verrugio, Claudio

Subjects

*MUSCULAR atrophy, *ANGIOTENSINS, *ENDOTOXINS, *SKELETAL muscle physiology, *MITOGEN-activated protein kinases, *SEPSIS, *LIPOPOLYSACCHARIDES, *THERAPEUTICS

Abstract

Skeletal muscle atrophy induced during sepsis syndrome produced by endotoxin in the form of LPS (lipopolysaccharide), is a pathological condition characterized by the loss of strength and muscle mass, an increase in MHC (myosin heavy chain) degradation, and an increase in the expression of atrogin-1 and MuRF-1 (muscle-specific RING-finger protein 1), two ubiquitin E3 ligases belonging to the ubiquitin-proteasome system. Ang-(1-7) [Angiotensin-(1-7)], through its Mas receptor, has beneficial effects in skeletal muscle. We evaluated in vivo the role of Ang-(1-7) and Mas receptor on the muscle wasting induced by LPS injection into C57BL/10J mice. In vitro studies were performed in murine C2C12 myotubes and isolated myofibres from EDL (extensor digitorum longus) muscle. In addition, the participation of p38 MAPK (mitogen-activated protein kinase) in the Ang-(1-7) effect on the LPS-induced muscle atrophy was evaluated. Our results show that Ang-(1-7) prevents the decrease in the diameter of myofibres and myotubes, the decrease in muscle strength, the diminution in MHC levels and the induction of atrogin-1 and MuRF-1 expression, all of which are induced by LPS. These effects were reversed by using A779, a Mas antagonist. Ang-(1-7) exerts these anti-atrophic effects at least in part by inhibiting the LPS-dependent activation of p38 MAPK both in vitro and in vivo. We have demonstrated for the first time that Ang-(1-7) counteracts the skeletal muscle atrophy induced by endotoxin through a mechanism dependent on the Mas receptor that involves a decrease in p38 MAPK phosphorylation. The present study indicates that Ang-(1-7) is a novel molecule with a potential therapeutic use to improve muscle wasting during endotoxin-induced sepsis syndrome. [ABSTRACT FROM AUTHOR]

Published

2015

2. Angiotensin type 2 receptor (AT2R) and receptor Mas: a complex liaison.

Author

Villela, Daniel, Leonhardt, Julia, Patel, Neal, Joseph, Jason, Kirsch, Sebastian, Hallberg, Anders, Unger, Thomas, Bader, Michael, Santos, Robson A., Sumners, Colin, and Steckelings, U. Muscha

Subjects

*ANGIOTENSIN receptors, *RENIN-angiotensin system, *CELLULAR signal transduction, *G protein coupled receptors, *DIMERIZATION, *METABOLITES, *LIGANDS (Biochemistry)

Abstract

The angiotensin type 2 receptor (AT2R) and the receptor Mas are components of the protective arms of the renin-angiotensin system (RAS), i.e. they both mediate tissue protective and regenerative actions. The spectrum of actions of these two receptors and their signalling mechanisms display striking similarities. Moreover, in some instances, antagonists for one receptor are able to inhibit the action of agonists for the respective other receptor. These observations suggest that there may be a functional or even physical interaction of both receptors. This article discusses potential mechanisms underlying the phenomenon of blockade of angiotensin-(1-7) [Ang-(1-7)] actions byAT2R antagonists and vice versa. Such mechanisms may comprise dimerization of the receptors or dimerization-independent mechanisms such as lack of specificity of the receptor ligands used in the experiments or involvement of the Ang-(1-7) metabolite alamandine and its receptor MrgD in the observed effects. We conclude that evidence for a functional interaction of both receptors is strong, but that such an interaction may be speciesand/ or tissue-specific and that elucidation of the precise nature of the interaction is only at the very beginning. [ABSTRACT FROM AUTHOR]

Published

2015

3. Protective axis of the renin–angiotensin system in the brain.

Author

GIRONACCI, Mariela M., CERNIELLO, Flavia M., LONGO CARBAJOSA, Nadia A., GOLDSTEIN, Jorge, and CERRATO, Bruno D.

Abstract

The RAS (renin–angiotensin system) is composed of two arms: the pressor arm containing AngII (angiotensin II)/ACE (angiotensin-converting enzyme)/AT1Rs (AngII type 1 receptors), and the depressor arm represented by Ang-(1–7) [angiotensin-(1–7)]/ACE2/Mas receptors. All of the components of the RAS are present in the brain. Within the brain, Ang-(1–7) contributes to the regulation of BP (blood pressure) by acting at regions that control cardiovascular function such that, when Ang-(1–7) is injected into the nucleus of the solitary tract, caudal ventrolateral medulla, paraventricular nucleus or anterior hypothalamic area, a reduction in BP occurs; however, when injected into the rostral ventrolateral medulla, Ang-(1–7) stimulates an increase in BP. In contrast with AngII, Ang-(1–7) improves baroreflex sensitivity and has an inhibitory neuromodulatory role in hypothalamic noradrenergic neurotransmission. Ang-(1–7) not only exerts effects related to BP regulation, but also acts as a cerebroprotective component of the RAS by reducing cerebral infarct size and neuronal apoptosis. In the present review, we provide an overview of effects elicited by Ang-(1–7) in the brain, which suggest a potential role for Ang-(1–7) in controlling the central development of hypertension. [ABSTRACT FROM AUTHOR]

Published

2014

4. Modulation of the action of insulin by angiotensin-(1-7).

Author

DOMINICI, Fernando P., BURGHI, Valeria, MUÑOZ, Marina C., and GIANI, Jorge F.

Subjects

*TYPE 2 diabetes treatment, *INSULIN resistance, *ANGIOTENSINS, *ANGIOTENSIN converting enzyme, *RENIN-angiotensin system, *METABOLIC syndrome treatment, *CELLULAR signal transduction

Abstract

The prevalence of Type 2 diabetes mellitus is predicted to increase dramatically over the coming years and the clinical implications and healthcare costs from this disease are overwhelming. In many cases, this pathological condition is linked to a cluster of metabolic disorders, such as obesity, systemic hypertension and dyslipidaemia, defined as the metabolic syndrome. Insulin resistance has been proposed as the key mediator of all of these features and contributes to the associated high cardiovascular morbidity and mortality. Although the molecular mechanisms behind insulin resistance are not completely understood, a negative cross-talk between AngII (angiotensin II) and the insulin signalling pathway has been the focus of great interest in the last decade. Indeed, substantial evidence has shown that anti-hypertensive drugs that block the RAS (renin-angiotensin system) may also act to prevent diabetes. Despite its long history, new components within the RAS continue to be discovered. Among them, Ang-(1-7) [angiotensin-(1-7)] has gained special attention as a counter-regulatory hormone opposing many of the AngII-related deleterious effects. Specifically, we and others have demonstrated that Ang-(1-7) improves the action of insulin and opposes the negative effect that AngII exerts at this level. In the present review, we provide evidence showing that insulin and Ang-(1-7) share a common intracellular signalling pathway. We also address the molecular mechanisms behind the beneficial effects of Ang-(1-7) on AngII-mediated insulin resistance. Finally, we discuss potential therapeutic approaches leading to modulation of the ACE2 (angiotensin-converting enzyme 2)/Ang-(1-7)/Mas receptor axis as a very attractive strategy in the therapy of the metabolic syndrome and diabetes-associated diseases. [ABSTRACT FROM AUTHOR]

Published

2014

5. Cerebroprotective action of angiotensin peptides in stroke.

Author

REGENHARDT, Robert W., BENNION, Douglas M., and SUMNERS, Colin

Subjects

*ANGIOTENSINS, *ANGIOTENSIN converting enzyme, *PATHOLOGICAL physiology, *ENZYME inhibitors, *HEMORRHAGIC diseases

Abstract

The goal of the present review is to examine the evidence for beneficial actions of manipulation of the RAS (renin–angiotensin system) in stroke, with particular focus on Ang-(1–7) [angiotensin-(1–7)] and its receptor Mas. The RAS appears to be highly involved in the multifactorial pathophysiology of stroke. Blocking the effects of AngII (angiotensin II) at AT1R (AngII type 1 receptor), through the use of commonly prescribed ACE (angiotensin-converting enzyme) inhibitors or AT1R blockers, has been shown to have therapeutic effects in both ischaemic and haemorrhagic stroke. In contrast with the deleterious actions of over activation of AT1R by AngII, stimulation of AT2Rs (AngII type 2 receptors) in the brain has been demonstrated to elicit beneficial effects in stroke. Likewise, the ACE2/Ang-(1–7)/Mas axis of the RAS has been shown to have therapeutic effects in stroke when activated, countering the effects of the ACE/AngII/AT1R axis. Studies have demonstrated that activating this axis in the brain elicits beneficial cerebral effects in rat models of ischaemic stroke, and we have also demonstrated the cerebroprotective potential of this axis in haemorrhagic stroke using stroke-prone spontaneously hypertensive rats and collagenase-induced striatal haemorrhage. The mechanism of cerebroprotection elicited by ACE2/Ang-(1–7)/Mas activation includes anti-inflammatory effects within the brain parenchyma. The major hurdle to overcome in translating these results to humans is devising strategies to activate the ACE2/Ang-(1–7)/Mas cerebroprotective axis using post-stroke treatments that can be administered non-invasively. [ABSTRACT FROM AUTHOR]

Published

2014

6. Angiotensin II type 1 receptor blockade restores angiotensin-(1-7)-induced coronary vasodilation in hypertrophic rat hearts.

Author

SOUZA, Álvaro P. S., SOBRINHO, Deny B. S., ALMEIDA, Jônathas F. Q., ALVES, Gisele M. M., MACEDO, Larissa M., PORTO, Juliana E., VÊNCIO, Eneida F., COLUGNATI, Diego B., SANTOS, Robson A. S., FERREIRA, Anderson J., MENDES, Elizabeth P., and CASTRO, Carlos H.

Subjects

*VASODILATION, *CARDIAC hypertrophy, *ANGIOTENSIN converting enzyme, *CORONARY disease, *LOSARTAN, *ANGIOTENSIN receptors, *HEART dilatation, *GUANYLATE cyclase

Abstract

The aim of the present study was to investigate the coronary effects of Ang-(1-7) [angiotensin-(1-7)] in hypertrophic rat hearts. Heart hypertrophy was induced by abdominal aorta CoA (coarctation). Ang-(1-7) and AVE 0991, a non-peptide Mas-receptor agonist, at picomolar concentration, induced a significant vasodilation in hearts from sham-operated rats. These effects were blocked by the Mas receptor antagonist A-779. Pre-treatment with L-NAME (N(G)-nitro-L-arginine methyl ester) or ODQ (1H-[1,2,4]oxadiazolo[4,3-a]quinozalin-1-one) [NOS (NO synthase) and soluble guanylate cyclase inhibitors respectively] also abolished the effect of Ang-(1-7) in control hearts. The coronary vasodilation produced by Ang-(1-7) and AVE 0991 was completely blunted in hypertrophic hearts. Chronic oral administration of losartan in CoA rats restored the coronary vasodilation effect of Ang-(1-7). This effect was blocked by A-779 and AT2 receptor (angiotensin II type 2 receptor) antagonist PD123319. Acute pre-incubation with losartan also restored the Ang-(1-7)-induced, but not BK (bradykinin)-induced, coronary vasodilation in hypertrophic hearts. This effect was inhibited by A-779, PD123319 and L-NAME. Chronic treatment with losartan did not change the protein expression of Mas and AT2 receptor and ACE (angiotensin-converting enzyme) and ACE2 in coronary arteries from CoA rats, but induced a slight increase in AT2 receptor in aorta of these animals. Ang-(1-7)-induced relaxation in aortas from sham-operated rats was absent in aortas from CoA rats. In vitro pre-treatment with losartan restored the Ang-(1-7)-induced relaxation in aortic rings of CoA rats, which was blocked by the Mas antagonist A-779 and L-NAME. These data demonstrate that Mas is strongly involved in coronary vasodilation and that AT1 receptor (angiotensin II type 1 receptor) blockade potentiates the vasodilatory effects of Ang-(1-7) in the coronary beds of pressure-overloaded rat hearts through NO-related AT2- and Mas-receptor-dependent mechanisms. These data suggest the association of Ang-(1-7) and AT1 receptor antagonists as a potential therapeutic avenue for coronary artery diseases. [ABSTRACT FROM AUTHOR]

Published

2013

7. Neuromodulatory role of angiotensin-(1-7) in the central nervous system.

Author

GIRONACCI, Mariela M., LONGO CARBAJOSA, Nadia A., GOLDSTEIN, Jorge, and CERRATO, Bruno D.

Subjects

*NEOVASCULARIZATION, *GROWTH associated protein-43, *ANGIOTENSINS, *CENTRAL nervous system, *TYROSINE hydroxylase, *SYNAPSES, *HYPERTENSION

Abstract

Ang-(1-7) [angiotensin-(1-7)] constitutes an important functional end-product of the RAS (renin-angiotensin system) endogenously formed from AngI (angiotensin I) or AngII (angiotensin II) through the catalytic activity of ACE2 (angiotensin-converting enzyme 2), prolyl carboxypeptidase, neutral endopeptidase or other endopeptidases. Ang-(1-7) lacks the pressor, dipsogenic or stimulatory effect on aldosterone release characteristic of AngII. In contrast, it produces vasodilation, natriuresis and diuresis, and inhibits angiogenesis and cell growth. At the central level, Ang-(1-7) acts at sites involved in the control of cardiovascular function, thus contributing to blood pressure regulation. This action may result from its inhibitory neuromodulatory action on NE [noradrenaline (norepinephrine)] levels at the synaptic cleft, i.e. Ang-(1-7) reduces NE release and synthesis, whereas it causes an increase in NE transporter expression, contributing in this way to central NE neuromodulation. Thus, by selective neurotransmitter release, Ang-(1-7) may contribute to the overall central cardiovascular effects. In the present review, we summarize the central effects of Ang-(1-7) and the mechanism by which the peptide modulates NE levels in the synaptic cleft. We also provide new evidences of its cerebroprotective role. [ABSTRACT FROM AUTHOR]

Published

2013

8. Angiotensin-(1-7): beyond the cardio-renal actions.

Author

PASSOS-SILVA, Danielle G., VERANO-BRAGA, Thiago, and SANTOS, Robson A. S.

Subjects

*ANGIOTENSINS, *RENIN-angiotensin system, *ANGIOTENSIN converting enzyme, *PHOSPHOINOSITIDE-dependent kinase-1, *EXTRACELLULAR signal-regulated kinases, *FORKHEAD transcription factors, *INFLAMMATION, *FIBROSIS

Abstract

is well known that the RAS (renin-angiotensin system) plays a key role in the modulation of many functions in the body. AngII (angiotensin II) acting on AT1R (type 1 AngII receptor) has a central role in mediating most of the actions of the RAS. However, over the past 10 years, several studies have presented evidence for the existence of a new arm of the RAS, namely the ACE (angiotensin-converting enzyme) 2/Ang-(1-7) [angiotensin-(1-7)]/Mas axis. Ang-(1-7) can be produced from AngI or AngII via endo- or carboxy-peptidases respectively. ACE2 appears to play a central role in Ang-(1-7) formation. As described for AngII, Ang-(1-7) also has a broad range of effects in different organs and tissues which goes beyond its initially described cardiovascular and renal actions. Those effects are mediated by Mas and can counter-regulate most of the deleterious effects of AngII. The interaction Ang-(1-7)/Mas regulates different signalling pathways, such as PI3K (phosphoinositide 3-kinase)/AKT and ERK (extracellularsignal- regulated kinase) pathways and involves downstream effectors such as NO, FOXO1 (forkhead box O1) and COX-2 (cyclo-oxygenase-2). Through these mechanisms, Ang-(1-7) is able to improve pathological conditions including fibrosis and inflammation in organs such as lungs, liver and kidney. In addition, this heptapeptide has positive effects on metabolism, increasing the glucose uptake and lipolysis while decreasing insulin resistance and dyslipidaemia. Ang-(1-7) is also able to improve cerebroprotection against ischaemic stroke, besides its effects on learning and memory. The reproductive system can also be affected by Ang-(1-7) treatment, with enhanced ovulation, spermatogenesis and sexual steroids synthesis. Finally, Ang-(1-7) is considered a potential anti-cancer treatment since it is able to inhibit cell proliferation and angiogenesis. Thus the ACE2/Ang-(1-7)/Mas pathway seems to be involved in many physiological and pathophysiological processes in several systems and organs especially by opposing the detrimental effects of inappropriate overactivation of the ACE/AngII/AT1R [ABSTRACT FROM AUTHOR]

Published

2013

9. The renin-angiotensin system, bone marrow and progenitor cells.

Author

DURIK, Matej, SEVÁ PESSÔA, Bruno, and ROKS, Anton J. M.

Subjects

*RENIN-angiotensin system, *ANGIOTENSIN receptors, *BONE marrow cells, *PROGENITOR cells, *HORMONES, *ANGIOTENSIN II, *DRUG therapy, *CARDIOVASCULAR system, *HYPERTROPHY, *DIURESIS, *REGENERATION (Biology)

Abstract

Modulation of the RAS (renin-angiotensin system), in particular of the function of the hormones AngII (angiotensin II) and Ang-(1-7) [angiotensin-(1-7)], is an important target for pharmacotherapy in the cardiovascular system. In the classical view, such modulation affects cardiovascular cells to decrease hypertrophy, fibrosis and endothelial dysfunction, and improves diuresis. In this view, excessive stimulation of AT1 receptors (AngII type 1 receptors) fulfils a detrimental role, as it promotes cardiovascular pathogenesis, and this is opposed by stimulation of the AT2 receptor (angiotensin II type 2 receptor) and the Ang-(1-7) receptor encoded by the Mas proto-oncogene. In recent years, this view has been broadened with the observation that the RAS regulates bone marrow stromal cells and stem cells, thus involving haematopoiesis and tissue regeneration by progenitor cells. This change of paradigm has enlarged the field of perspectives for therapeutic application of existing as well as newly developed medicines that alter angiotensin signalling, which now stretches beyond cardiovascular therapy. In the present article, we review the role of AngII and Ang-(1-7) and their respective receptors in haematopoietic and mesenchymal stem cells, and discuss possible pharmacotherapeutical implications. [ABSTRACT FROM AUTHOR]

Published

2012

10. Epochs in the depressor/pressor balance of the renin–angiotensin system

Author

Lucinda M Hilliard, Katrina M Mirabito Colafella, and Kate M. Denton

Subjects

0301 basic medicine, medicine.medical_specialty, Angiotensin receptor, Blood Pressure, Peptidyl-Dipeptidase A, 030204 cardiovascular system & hematology, Proto-Oncogene Mas, Renin-Angiotensin System, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Extracellular fluid, Renin–angiotensin system, medicine, Animals, Humans, Vasoconstrictor Agents, Receptor, Sex Characteristics, business.industry, Mas receptor, General Medicine, Angiotensin II, 030104 developmental biology, Endocrinology, Kidney Diseases, Angiotensin-Converting Enzyme 2, business, Homeostasis

Abstract

The renin–angiotensin system (RAS) plays a commanding role in the regulation of extracellular fluid homoeostasis. Tigerstadt and Bergman first identified the RAS more than two centuries ago. By the 1980s a voyage of research and discovery into the mechanisms and actions of this system led to the development of drugs that block the RAS, which have become the mainstay for the treatment of cardiovascular and renal disease. In the last 25 years new components of the RAS have come to light, including the angiotensin type 2 receptor (AT2R) and the angiotensin-converting enzyme 2 (ACE2)/angiotensin-(1–7) [Ang(1–7)]/Mas receptor (MasR) axis. These have been shown to counter the classical actions of angiotensin II (AngII) at the predominant angiotensin type 1 receptor (AT1R). Our studies, and those of others, have demonstrated that targeting these depressor RAS pathways may be therapeutically beneficial. It is apparent that the evolution of both the pressor and depressor RAS pathways is distinct throughout life and that the depressor/pressor balance of the RAS vary between the sexes. These temporal patterns of expression suggest that therapies targeting the RAS could be optimized for discrete epochs in life.

Published

2016

11. Reduction in renal ACE2 expression in subtotal nephrectomy in rats is ameliorated with ACE inhibition

Author

Vicki Levidiotis, Luke J. Burchill, Louise M Burrell, Rachael G Dean, and Elena Velkoska

Subjects

BP, blood pressure, angiotensin-(1–7), medicine.medical_treatment, Gene Expression, Angiotensin-Converting Enzyme Inhibitors, SBP, systolic BP, Nephrectomy, Proto-Oncogene Mas, Receptors, G-Protein-Coupled, Rats, Sprague-Dawley, Diabetic nephropathy, Random Allocation, Ramipril, Ang-(1–7), angiotensin(1–7), renin–angiotensin system (RAS), Kidney, biology, Chemistry, AngII, angiotensin II, Acute kidney injury, General Medicine, ARB, angiotensin receptor blocker, Proteinuria, medicine.anatomical_structure, Hypertension, STNx, subtotal nephrectomy, Female, Angiotensin-Converting Enzyme 2, hormones, hormone substitutes, and hormone antagonists, Research Article, FAM, 6-carboxyfluorescin, medicine.drug, kidney, medicine.medical_specialty, renal injury, ACE, angiotensin-converting enzyme, QRT–PCR, quantitative real-time–PCR, Peptidyl-Dipeptidase A, STZ, streptozotocin, TAMRA, 6-carboxytetramethylrhodamine, RAS, renin–angiotensin system, Proto-Oncogene Proteins, Internal medicine, medicine, Animals, mas receptor, Polyuria, Angiotensin-converting enzyme, medicine.disease, Angiotensin II, BCA, bicinchoninic acid, QFS, quenched fluorescent substrate, Rats, Endocrinology, biology.protein, ACEI, ACE inhibitor, Kidney disease

Abstract

Alterations within the RAS (renin–angiotensin system) are pivotal for the development of renal disease. ACE2 (angiotensin-converting enzyme 2) is expressed in the kidney and converts the vasoconstrictor AngII (angiotensin II) into Ang-(1–7), a peptide with vasodilatory and anti-fibrotic actions. Although the expression of ACE2 in the diabetic kidney has been well studied, little is known about its expression in non-diabetic renal disease. In the present study, we assessed ACE2 in rats with acute kidney injury induced by STNx (subtotal nephrectomy). STNx and Control rats received vehicle or ramipril (1 mg·kg−1 of body weight·day−1), and renal ACE, ACE2 and mas receptor gene and protein expression were measured 10 days later. STNx rats were characterized by polyuria, proteinuria, hypertension and elevated plasma ACE2 activity (all P

Published

2009