Restoration of muscle strength in dystrophic muscle by angiotensin-1-7 through inhibition of TGF-β signalling

Acuña, María José; Pessina, Patrizia; Olguín, Hugo C.; Cabrera, Daniel; Vio, Carlos P.; Bäder, Michael; Muñoz‐Cánoves, Pura; Santos, Robson A.S.; Cabello-Verrugio, Claudio; Brandan, Enrique

doi:10.1093/hmg/ddt514

Cited by 143 publications

(181 citation statements)

References 56 publications

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“…In contrast to the present study, Ferreira et al showed an improved cardiac function, indicated by elevated dp/dt anddp/dt and furthermore, an attenuation of the isoproterenolinduced cardiac fibrosis in transgenic rats. Previous studies also indicated an antifibrotic action of Ang(1-7) in vitro and in vivo (Santos et al, 2004;Ferreira et al, 2010;Dong et al, 2012;McCollum et al, 2012;Acuña et al, 2014). In contrast to these findings, the present study revealed no antifibrotic effect of Ang(1-7) in a transgenic rat model.…”

Section: Discussioncontrasting

confidence: 88%

Effect of Angiotensin (1-7) on Heart Function in an Experimental Rat Model of Obesity

Blanke¹,

Schlegel²,

Salameh³

et al. 2016

Thorac cardiovasc Surg

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Aim: Obesity is a risk factor for the development of cardiovascular diseases. Recently it was shown that overexpression of the Mas-receptor antagonist angiotensin(1-7) could prevent from diet-induced obesity. However, it remained unclear whether diet-induced obesity and angiotensin(1-7) overexpression might also have effects on the cardiovascular system in these rats.Methods: Twenty three male Sprague Dawley rats were fed with standard chow (SD+chow, n = 5) or a cafeteria diet (SD+CD, n = 6) for 5 months. To investigate the effect of angiotensin(1-7) transgenic rats, expressing an angiotensin(1-7)-producing fusion protein in testis were used. These transgenic rats also received a 5 month's feeding period with either chow (TGR+chow, n = 6) or cafeteria diet (TGR+CD, n = 6), respectively. Hemodynamic measurements (pressure-volume loops) were carried out to assess cardiac function and blood pressure. Subsequently, hearts were explanted and investigated according to the Langendorff technique. Furthermore, cardiac remodeling in these animals was investigated histologically.Results: After 5 months cafeteria diet feeding rats showed a significantly increased body weight, which could be prevented in transgenic rats. However, there was no effect on cardiac performance after cafeteria diet in non-transgenic and transgenic rats. Moreover, overexpression of angiotensin(1-7) deteriorated cardiac contractility as indicated by impaired dp/dt. Furthermore, histological analysis revealed that cafeteria diet led to myocardial fibrosis in both, control and transgenic rats and this was not inhibited by an overproduction of angiotensin(1-7). Conclusion:These results indicate that an overexpression of circulating angiotensin(1-7) prevents a cafeteria diet-induced increase in body weight, but does not affect cardiac performance in this experimental rat model of obesity. Furthermore, overexpression of angiotensin(1-7) alone resulted in an impairment of cardiac function.

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Section: Discussioncontrasting

confidence: 88%

Effect of Angiotensin (1-7) on Heart Function in an Experimental Rat Model of Obesity

Blanke¹,

Schlegel²,

Salameh³

et al. 2016

Thorac cardiovasc Surg

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“…Fibrous tissues may prevent normal tissue recovery, particularly in the muscle where fibrosis has been shown to lead to progressive skeletal muscle injury, for example in Duchenne's muscular dystrophy (Acuna et al, 2014). Previous work has suggested that PDGFRβ+ pericytes contribute to scar formation (Arimura et al, 2012) and express fibroblast-associated markers (such as collagen IV, fibronectin and fibroblast surface proteins).…”

Section: Tissue Fibrosismentioning

confidence: 99%

Pericytes, mesenchymal stem cells and their contributions to tissue repair

Wong

Rowley

Redpath

et al. 2015

Pharmacology & Therapeutics

143

102

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Regenerative medicine using mesenchymal stem cells for the purposes of tissue repair has garnered considerable public attention due to the potential of returning tissues and organs to a normal, healthy state after injury or damage has occurred. To achieve this, progenitor cells such as pericytes and bone marrow-derived mesenchymal stem cells can be delivered exogenously, mobilised and recruited from within the body or transplanted in the form organs and tissues grown in the laboratory from stem cells. In this review, we summarise the recent evidence supporting the use of endogenously mobilised stem cell populations to enhance tissue repair along with the use of mesenchymal stem cells and pericytes in the development of engineered tissues. Finally, we conclude with an overview of currently available therapeutic options to manipulate endogenous stem cells to promote tissue repair.

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“…However, the instability of Ang-(1-7) restricts efficient oral or injected administration. 11,19 A new delivery method is needed that increases the half-life and improves the bioavailability of this peptide in target tissues.…”

Section: Introductionmentioning

confidence: 99%

The complex of PAMAM-OH dendrimer with Angiotensin (1–7) prevented the disuse-induced skeletal muscle atrophy in mice

Márquez-Miranda

Ábrigo

Rivera

et al. 2017

IJN

Self Cite

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Angiotensin (1–7) (Ang-(1–7)) is a bioactive heptapeptide with a short half-life and has beneficial effects in several tissues – among them, skeletal muscle – by preventing muscle atrophy. Dendrimers are promising vehicles for the protection and transport of numerous bioactive molecules. This work explored the use of a neutral, non-cytotoxic hydroxyl-terminated poly(amidoamine) (PAMAM-OH) dendrimer as an Ang-(1–7) carrier. Bioinformatics analysis showed that the Ang-(1–7)-binding capacity of the dendrimer presented a 2:1 molar ratio. Molecular dynamics simulation analysis revealed the capacity of neutral PAMAM-OH to protect Ang-(1–7) and form stable complexes. The peptide coverage ability of the dendrimer was between ~50% and 65%. Furthermore, an electrophoretic mobility shift assay demonstrated that neutral PAMAM-OH effectively bonded peptides. Experimental results showed that the Ang-(1–7)/PAMAM-OH complex, but not Ang-(1–7) alone, had an anti-atrophic effect when administered intraperitoneally, as evaluated by muscle strength, fiber diameter, myofibrillar protein levels, and atrogin-1 and MuRF-1 expressions. The results of the Ang-(1–7)/PAMAM-OH complex being intraperitoneally injected were similar to the results obtained when Ang-(1–7) was systemically administered through mini-osmotic pumps. Together, the results suggest that Ang-(1–7) can be protected for PAMAM-OH when this complex is intraperitoneally injected. Therefore, the Ang-(1–7)/PAMAM-OH complex is an efficient delivery method for Ang-(1–7), since it improves the anti-atrophic activity of this peptide in skeletal muscle.

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Restoration of muscle strength in dystrophic muscle by angiotensin-1-7 through inhibition of TGF-β signalling

Cited by 143 publications

References 56 publications

Effect of Angiotensin (1-7) on Heart Function in an Experimental Rat Model of Obesity

Effect of Angiotensin (1-7) on Heart Function in an Experimental Rat Model of Obesity

Pericytes, mesenchymal stem cells and their contributions to tissue repair

The complex of PAMAM-OH dendrimer with Angiotensin (1–7) prevented the disuse-induced skeletal muscle atrophy in mice

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Restoration of muscle strength in dystrophic muscle by angiotensin-1-7 through inhibition of TGF-β signalling

Cited by 143 publications

References 56 publications

Effect of Angiotensin (1-7) on Heart Function in an Experimental Rat Model of Obesity

Effect of Angiotensin (1-7) on Heart Function in an Experimental Rat Model of Obesity

Pericytes, mesenchymal stem cells and their contributions to tissue repair

The complex of PAMAM-OH dendrimer with Angiotensin (1&ndash;7) prevented the disuse-induced skeletal muscle atrophy in mice

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Product

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The complex of PAMAM-OH dendrimer with Angiotensin (1–7) prevented the disuse-induced skeletal muscle atrophy in mice