Your search keyword '"Winbanks, Catherine E."' showing total 20 results

1. Perturbed BMP signaling and denervation promote muscle wasting in cancer cachexia.

Author

Sartori R, Hagg A, Zampieri S, Armani A, Winbanks CE, Viana LR, Haidar M, Watt KI, Qian H, Pezzini C, Zanganeh P, Turner BJ, Larsson A, Zanchettin G, Pierobon ES, Moletta L, Valmasoni M, Ponzoni A, Attar S, Da Dalt G, Sperti C, Kustermann M, Thomson RE, Larsson L, Loveland KL, Costelli P, Megighian A, Merigliano S, Penna F, Gregorevic P, and Sandri M

Subjects

Animals, Denervation, Humans, Mice, Muscle, Skeletal pathology, Muscular Atrophy, Cachexia, Neoplasms complications, Neoplasms pathology

Abstract

Most patients with advanced solid cancers exhibit features of cachexia, a debilitating syndrome characterized by progressive loss of skeletal muscle mass and strength. Because the underlying mechanisms of this multifactorial syndrome are incompletely defined, effective therapeutics have yet to be developed. Here, we show that diminished bone morphogenetic protein (BMP) signaling is observed early in the onset of skeletal muscle wasting associated with cancer cachexia in mouse models and in patients with cancer. Cancer-mediated factors including Activin A and IL-6 trigger the expression of the BMP inhibitor Noggin in muscle, which blocks the actions of BMPs on muscle fibers and motor nerves, subsequently causing disruption of the neuromuscular junction (NMJ), denervation, and muscle wasting. Increasing BMP signaling in the muscles of tumor-bearing mice by gene delivery or pharmacological means can prevent muscle wasting and preserve measures of NMJ function. The data identify perturbed BMP signaling and denervation of muscle fibers as important pathogenic mechanisms of muscle wasting associated with tumor growth. Collectively, these findings present interventions that promote BMP-mediated signaling as an attractive strategy to counteract the loss of functional musculature in patients with cancer., (Copyright © 2021 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2021

2. Old Drug, New Trick: Tilorone, a Broad-Spectrum Antiviral Drug as a Potential Anti-Fibrotic Therapeutic for the Diseased Heart.

Author

Horlock D, Kaye DM, Winbanks CE, Gao XM, Kiriazis H, Donner DG, Gregorevic P, McMullen JR, and Bernardo BC

Abstract

Cardiac fibrosis is associated with most forms of cardiovascular disease. No reliable therapies targeting cardiac fibrosis are available, thus identifying novel drugs that can resolve or prevent fibrosis is needed. Tilorone, an antiviral agent, can prevent fibrosis in a mouse model of lung disease. We investigated the anti-fibrotic effects of tilorone in human cardiac fibroblasts in vitro by performing a radioisotopic assay for [ 3 H]-proline incorporation as a proxy for collagen synthesis. Exploratory studies in human cardiac fibroblasts treated with tilorone (10 µM) showed a significant reduction in transforming growth factor-β induced collagen synthesis compared to untreated fibroblasts. To determine if this finding could be recapitulated in vivo, mice with established pathological remodelling due to four weeks of transverse aortic constriction (TAC) were administered tilorone (50 mg/kg, i.p) or saline every third day for eight weeks. Treatment with tilorone was associated with attenuation of fibrosis (assessed by Masson's trichrome stain), a favourable cardiac gene expression profile and no further deterioration of cardiac systolic function determined by echocardiography compared to saline treated TAC mice. These data demonstrate that tilorone has anti-fibrotic actions in human cardiac fibroblasts and the adult mouse heart, and represents a potential novel therapy to treat fibrosis associated with heart failure.

Published

2021

3. Smad7 gene delivery prevents muscle wasting associated with cancer cachexia in mice.

Author

Winbanks CE, Murphy KT, Bernardo BC, Qian H, Liu Y, Sepulveda PV, Beyer C, Hagg A, Thomson RE, Chen JL, Walton KL, Loveland KL, McMullen JR, Rodgers BD, Harrison CA, Lynch GS, and Gregorevic P

Subjects

Activin Receptors, Type II genetics, Activin Receptors, Type II metabolism, Animals, Blotting, Western, Mice, Muscle Proteins genetics, Muscle Proteins metabolism, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Muscular Atrophy etiology, Myocardium metabolism, Myocardium pathology, Neoplasms complications, Neoplasms metabolism, Phosphorylation genetics, Phosphorylation physiology, SKP Cullin F-Box Protein Ligases genetics, SKP Cullin F-Box Protein Ligases metabolism, Signal Transduction genetics, Signal Transduction physiology, Smad2 Protein genetics, Smad2 Protein metabolism, Smad3 Protein genetics, Smad3 Protein metabolism, Smad7 Protein genetics, Tripartite Motif Proteins genetics, Tripartite Motif Proteins metabolism, Ubiquitin-Protein Ligases genetics, Ubiquitin-Protein Ligases metabolism, Muscular Atrophy metabolism, Muscular Atrophy therapy, Neoplasms physiopathology, Smad7 Protein metabolism

Abstract

Patients with advanced cancer often succumb to complications arising from striated muscle wasting associated with cachexia. Excessive activation of the type IIB activin receptor (ActRIIB) is considered an important mechanism underlying this wasting, where circulating procachectic factors bind ActRIIB and ultimately lead to the phosphorylation of SMAD2/3. Therapeutics that antagonize the binding of ActRIIB ligands are in clinical development, but concerns exist about achieving efficacy without off-target effects. To protect striated muscle from harmful ActRIIB signaling, and to reduce the risk of off-target effects, we developed an intervention using recombinant adeno-associated viral vectors (rAAV vectors) that increase expression of Smad7 in skeletal and cardiac muscles. SMAD7 acts as an intracellular negative regulator that prevents SMAD2/3 activation and promotes degradation of ActRIIB complexes. In mouse models of cachexia, rAAV:Smad7 prevented wasting of skeletal muscles and the heart independent of tumor burden and serum levels of procachectic ligands. Mechanistically, rAAV:Smad7 administration abolished SMAD2/3 signaling downstream of ActRIIB and inhibited expression of the atrophy-related ubiquitin ligases MuRF1 and MAFbx. These findings identify muscle-directed Smad7 gene delivery as a potential approach for preventing muscle wasting under conditions where excessive ActRIIB signaling occurs, such as cancer cachexia., (Copyright © 2016, American Association for the Advancement of Science.)

Published

2016

4. Evaluation of follistatin as a therapeutic in models of skeletal muscle atrophy associated with denervation and tenotomy.

Author

Sepulveda PV, Lamon S, Hagg A, Thomson RE, Winbanks CE, Qian H, Bruce CR, Russell AP, and Gregorevic P

Subjects

Animals, Dependovirus genetics, Disease Models, Animal, Follistatin metabolism, Gene Expression, Gene Transfer Techniques, Genetic Vectors administration & dosage, Genetic Vectors genetics, Hypertrophy, Mice, Muscle, Skeletal innervation, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Muscular Atrophy therapy, Signal Transduction, TOR Serine-Threonine Kinases metabolism, Transduction, Genetic, Denervation adverse effects, Follistatin genetics, Genetic Therapy, Muscular Atrophy etiology, Muscular Atrophy pathology, Tenotomy adverse effects

Abstract

Follistatin is an inhibitor of TGF-β superfamily ligands that repress skeletal muscle growth and promote muscle wasting. Accordingly, follistatin has emerged as a potential therapeutic to ameliorate the deleterious effects of muscle atrophy. However, it remains unclear whether the anabolic effects of follistatin are conserved across different modes of non-degenerative muscle wasting. In this study, the delivery of a recombinant adeno-associated viral vector expressing follistatin (rAAV:Fst) to the hind-limb musculature of mice two weeks prior to denervation or tenotomy promoted muscle hypertrophy that was sufficient to preserve muscle mass comparable to that of untreated sham-operated muscles. However, administration of rAAV:Fst to muscles at the time of denervation or tenotomy did not prevent subsequent muscle wasting. Administration of rAAV:Fst to innervated or denervated muscles increased protein synthesis, but markedly reduced protein degradation only in innervated muscles. Phosphorylation of the signalling proteins mTOR and S6RP, which are associated with protein synthesis, was increased in innervated muscles administered rAAV:Fst, but not in treated denervated muscles. These results demonstrate that the anabolic effects of follistatin are influenced by the interaction between muscle fibres and motor nerves. These findings have important implications for understanding the potential efficacy of follistatin-based therapies for non-degenerative muscle wasting.

Published

2015

5. miR-21 promotes renal fibrosis in diabetic nephropathy by targeting PTEN and SMAD7.

Author

McClelland AD, Herman-Edelstein M, Komers R, Jha JC, Winbanks CE, Hagiwara S, Gregorevic P, Kantharidis P, and Cooper ME

Subjects

Animals, Apolipoproteins E deficiency, Apolipoproteins E genetics, Case-Control Studies, Cell Line, Collagen metabolism, Diabetes Mellitus, Experimental chemically induced, Diabetes Mellitus, Experimental complications, Diabetic Nephropathies etiology, Diabetic Nephropathies genetics, Diabetic Nephropathies pathology, Fibrosis, Glomerular Filtration Rate, Humans, Kidney Tubules, Proximal drug effects, Kidney Tubules, Proximal pathology, Kidney Tubules, Proximal physiopathology, Mice, Knockout, MicroRNAs genetics, Phosphorylation, Prognosis, Proto-Oncogene Proteins c-akt metabolism, RNA Interference, Rats, Sprague-Dawley, Severity of Illness Index, Signal Transduction, Smad7 Protein genetics, Transfection, Transforming Growth Factor beta1 pharmacology, Up-Regulation, Diabetic Nephropathies metabolism, Kidney Tubules, Proximal metabolism, MicroRNAs metabolism, PTEN Phosphohydrolase metabolism, Smad7 Protein metabolism

Abstract

The cytokine transforming growth factor (TGF)-β1 plays a central role in diabetic nephropathy (DN) with data implicating the miRNA (miR) miR-21 as a key modulator of its prosclerotic actions. In the present study, we demonstrate data indicating that miR-21 up-regulation positively correlates with the severity of fibrosis and rate of decline in renal function in human DN. Furthermore, concomitant analyses of various models of fibrotic renal disease and experimental DN, confirm tubular miR-21 up-regulation. The fibrotic changes associated with increased miR-21 levels are proposed to include the regulation of TGF-β1-mediated mothers against decapentaplegic homolog 3 (SMAD3)- and phosphoinositide 3-kinase (PI3K)-dependent signalling pathways via co-ordinated repression of mothers against decapentaplegic homolog 7 (SMAD7) and phosphatase and tensin homologue (PTEN) respectively. This represents a previously uncharacterized interaction axis between miR-21 and PTEN-SMAD7. Targeting of these proteins by miR-21 resulted in de-repression of the respective pathways as reflected by increases in SMAD3 and V-Akt murine thymoma viral oncogene homolog 1 (AKT) phosphorylation. Many of the changes typically induced by TGF-β1, including phosphorylation of signalling mediators, were further enhanced by miR-21. Collectively, these data present a unified model for a key role for miR-21 in the regulation of renal tubular extracellular matrix (ECM) synthesis and accumulation and provide important insights into the molecular pathways implicated in the progression of DN., (© 2015 Authors; published by Portland Press Limited.)

Published

2015

6. Therapeutic silencing of miR-652 restores heart function and attenuates adverse remodeling in a setting of established pathological hypertrophy.

Author

Bernardo BC, Nguyen SS, Winbanks CE, Gao XM, Boey EJ, Tham YK, Kiriazis H, Ooi JY, Porrello ER, Igoor S, Thomas CJ, Gregorevic P, Lin RC, Du XJ, and McMullen JR

Subjects

Animals, Cells, Cultured, Mice, Rats, Rats, Sprague-Dawley, Real-Time Polymerase Chain Reaction, Cardiomegaly genetics, Gene Silencing, Heart physiopathology, MicroRNAs genetics

Abstract

Expression of microRNA-652 (miR-652) increases in the diseased heart, decreases in a setting of cardioprotection, and is inversely correlated with heart function. The aim of this study was to assess the therapeutic potential of inhibiting miR-652 in a mouse model with established pathological hypertrophy and cardiac dysfunction due to pressure overload. Mice were subjected to a sham operation or transverse aortic constriction (TAC) for 4 wk to induce hypertrophy and cardiac dysfunction, followed by administration of a locked nucleic acid (LNA)-antimiR-652 (miR-652 inhibitor) or LNA control. Cardiac function was assessed before and 8 wk post-treatment. Expression of miR-652 increased in hearts subjected to TAC compared to sham surgery (2.9-fold), and this was suppressed by ∼95% in LNA-antimiR-652-treated TAC mice. Inhibition of miR-652 improved cardiac function in TAC mice (fractional shortening:29±1% at 4 wk post-TAC compared to 35±1% post-treatment) and attenuated cardiac hypertrophy. Improvement in heart function was associated with reduced cardiac fibrosis, less apoptosis and B-type natriuretic peptide gene expression, and preserved angiogenesis. Mechanistically, we identified Jagged1 (a Notch1 ligand) as a novel direct target of miR-652. In summary, these studies provide the first evidence that silencing of miR-652 protects the heart against pathological remodeling and improves heart function., (© FASEB.)

Published

2014

7. MicroRNAs differentially regulated in cardiac and skeletal muscle in health and disease: potential drug targets?

Author

Winbanks CE, Ooi JY, Nguyen SS, McMullen JR, and Bernardo BC

Subjects

Animals, Exercise physiology, Heart drug effects, Heart growth & development, Heart Diseases genetics, Heart Diseases metabolism, Humans, Muscle, Skeletal growth & development, Muscular Diseases genetics, Muscular Diseases metabolism, Health, Heart Diseases drug therapy, MicroRNAs genetics, MicroRNAs metabolism, Molecular Targeted Therapy methods, Muscle, Skeletal metabolism, Muscular Diseases drug therapy, Myocardium metabolism

Abstract

The identification of non-coding RNA species, previously thought of as 'junk' DNA, adds a new dimension of complexity to the regulation of DNA, RNA and protein. MicroRNAs are short non-coding RNA species that control gene expression, are dysregulated in settings of cardiac and skeletal muscle disease and have emerged as promising therapeutic targets. MicroRNAs specifically enriched in cardiac and skeletal muscle are called myomiRs and play an important role in cardiac pathology and skeletal muscle biology. Moreover, microRNA profiles are altered in response to exercise and disease; thus, their potential as therapeutic drug targets is being widely explored. In the cardiovascular field, therapeutic inhibition of microRNAs has been shown to be effective in improving cardiac outcome in preclinical cardiac disease models. MicroRNAs that promote skeletal muscle regeneration are attractive therapeutic targets in muscle wasting conditions where regenerative capacity is compromised., (© 2014 Wiley Publishing Asia Pty Ltd.)

Published

2014

8. Elevated expression of activins promotes muscle wasting and cachexia.

Author

Chen JL, Walton KL, Winbanks CE, Murphy KT, Thomson RE, Makanji Y, Qian H, Lynch GS, Harrison CA, and Gregorevic P

Subjects

Activin Receptors, Type II genetics, Activin Receptors, Type II metabolism, Activins blood, Activins metabolism, Animals, Blotting, Western, Cachexia metabolism, Cell Line, Tumor, Cyclin-Dependent Kinase Inhibitor p21 genetics, Cyclin-Dependent Kinase Inhibitor p21 metabolism, Dependovirus genetics, Genetic Vectors genetics, Humans, MCF-7 Cells, Mice, Mice, Inbred C57BL, Mice, Knockout, Muscle Proteins genetics, Muscle Proteins metabolism, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Muscular Atrophy metabolism, Myostatin deficiency, Myostatin genetics, Reverse Transcriptase Polymerase Chain Reaction, SKP Cullin F-Box Protein Ligases genetics, SKP Cullin F-Box Protein Ligases metabolism, Signal Transduction genetics, Activins genetics, Cachexia genetics, Gene Expression, Muscular Atrophy genetics

Abstract

In models of cancer cachexia, inhibiting type IIB activin receptors (ActRIIBs) reverse muscle wasting and prolongs survival, even with continued tumor growth. ActRIIB mediates signaling of numerous TGF-β proteins; of these, we demonstrate that activins are the most potent negative regulators of muscle mass. To determine whether activin signaling in the absence of tumor-derived factors induces cachexia, we used recombinant serotype 6 adeno-associated virus (rAAV6) vectors to increase circulating activin A levels in C57BL/6 mice. While mice injected with control vector gained ~10% of their starting body mass (3.8±0.4 g) over 10 wk, mice injected with increasing doses of rAAV6:activin A exhibited weight loss in a dose-dependent manner, to a maximum of -12.4% (-4.2±1.1 g). These reductions in body mass in rAAV6:activin-injected mice correlated inversely with elevated serum activin A levels (7- to 24-fold). Mechanistically, we show that activin A reduces muscle mass and function by stimulating the ActRIIB pathway, leading to deleterious consequences, including increased transcription of atrophy-related ubiquitin ligases, decreased Akt/mTOR-mediated protein synthesis, and a profibrotic response. Critically, we demonstrate that the muscle wasting and fibrosis that ensues in response to excessive activin levels is fully reversible. These findings highlight the therapeutic potential of targeting activins in cachexia.

Published

2014

9. Silencing of miR-34a attenuates cardiac dysfunction in a setting of moderate, but not severe, hypertrophic cardiomyopathy.

Author

Bernardo BC, Gao XM, Tham YK, Kiriazis H, Winbanks CE, Ooi JY, Boey EJ, Obad S, Kauppinen S, Gregorevic P, Du XJ, Lin RC, and McMullen JR

Subjects

Animals, Cardiomyopathy, Hypertrophic pathology, Disease Models, Animal, Echocardiography, Fibrosis, Gene Expression Regulation, Male, Mice, Severity of Illness Index, Ventricular Remodeling genetics, Cardiomyopathy, Hypertrophic genetics, Cardiomyopathy, Hypertrophic physiopathology, Gene Silencing, MicroRNAs genetics

Abstract

Therapeutic inhibition of the miR-34 family (miR-34a,-b,-c), or miR-34a alone, have emerged as promising strategies for the treatment of cardiac pathology. However, before advancing these approaches further for potential entry into the clinic, a more comprehensive assessment of the therapeutic potential of inhibiting miR-34a is required for two key reasons. First, miR-34a has ∼40% fewer predicted targets than the miR-34 family. Hence, in cardiac stress settings in which inhibition of miR-34a provides adequate protection, this approach is likely to result in less potential off-target effects. Secondly, silencing of miR-34a alone may be insufficient in settings of established cardiac pathology. We recently demonstrated that inhibition of the miR-34 family, but not miR-34a alone, provided benefit in a chronic model of myocardial infarction. Inhibition of miR-34 also attenuated cardiac remodeling and improved heart function following pressure overload, however, silencing of miR-34a alone was not examined. The aim of this study was to assess whether inhibition of miR-34a could attenuate cardiac remodeling in a mouse model with pre-existing pathological hypertrophy. Mice were subjected to pressure overload via constriction of the transverse aorta for four weeks and echocardiography was performed to confirm left ventricular hypertrophy and systolic dysfunction. After four weeks of pressure overload (before treatment), two distinct groups of animals became apparent: (1) mice with moderate pathology (fractional shortening decreased ∼20%) and (2) mice with severe pathology (fractional shortening decreased ∼37%). Mice were administered locked nucleic acid (LNA)-antimiR-34a or LNA-control with an eight week follow-up. Inhibition of miR-34a in mice with moderate cardiac pathology attenuated atrial enlargement and maintained cardiac function, but had no significant effect on fetal gene expression or cardiac fibrosis. Inhibition of miR-34a in mice with severe pathology provided no therapeutic benefit. Thus, therapies that inhibit miR-34a alone may have limited potential in settings of established cardiac pathology.

Published

2014

10. The bone morphogenetic protein axis is a positive regulator of skeletal muscle mass.

Author

Winbanks CE, Chen JL, Qian H, Liu Y, Bernardo BC, Beyer C, Watt KI, Thomson RE, Connor T, Turner BJ, McMullen JR, Larsson L, McGee SL, Harrison CA, and Gregorevic P

Subjects

Animals, Bone Morphogenetic Protein 7 genetics, Bone Morphogenetic Protein Receptors, Type I metabolism, Dependovirus, Disease Models, Animal, Female, Follistatin metabolism, Genetic Therapy, Genetic Vectors, HEK293 Cells, Histone Deacetylases metabolism, Humans, Hypertrophy, Mice, Mice, Inbred C57BL, Muscle, Skeletal growth & development, Muscle, Skeletal innervation, Muscle, Skeletal pathology, Muscular Atrophy genetics, Muscular Atrophy metabolism, Muscular Atrophy pathology, Myogenin metabolism, Phosphorylation, Rats, Rats, Sprague-Dawley, Smad Proteins metabolism, TOR Serine-Threonine Kinases metabolism, Transduction, Genetic, Transfection, Ubiquitin-Protein Ligases metabolism, Bone Morphogenetic Protein 7 metabolism, Muscle Development, Muscle, Skeletal metabolism, Muscular Atrophy prevention & control, Signal Transduction

Abstract

Although the canonical transforming growth factor β signaling pathway represses skeletal muscle growth and promotes muscle wasting, a role in muscle for the parallel bone morphogenetic protein (BMP) signaling pathway has not been defined. We report, for the first time, that the BMP pathway is a positive regulator of muscle mass. Increasing the expression of BMP7 or the activity of BMP receptors in muscles induced hypertrophy that was dependent on Smad1/5-mediated activation of mTOR signaling. In agreement, we observed that BMP signaling is augmented in models of muscle growth. Importantly, stimulation of BMP signaling is essential for conservation of muscle mass after disruption of the neuromuscular junction. Inhibiting the phosphorylation of Smad1/5 exacerbated denervation-induced muscle atrophy via an HDAC4-myogenin-dependent process, whereas increased BMP-Smad1/5 activity protected muscles from denervation-induced wasting. Our studies highlight a novel role for the BMP signaling pathway in promoting muscle growth and inhibiting muscle wasting, which may have significant implications for the development of therapeutics for neuromuscular disorders.

Published

2013

11. miR-206 represses hypertrophy of myogenic cells but not muscle fibers via inhibition of HDAC4.

Author

Winbanks CE, Beyer C, Hagg A, Qian H, Sepulveda PV, and Gregorevic P

Subjects

Animals, Cell Line, Dependovirus genetics, Genetic Vectors genetics, Hypertrophy genetics, Mice, Muscle Fibers, Skeletal enzymology, Muscle Fibers, Skeletal physiology, Muscular Atrophy genetics, Histone Deacetylases genetics, MicroRNAs genetics, Muscle Development, Muscle Fibers, Skeletal cytology, Muscle Fibers, Skeletal pathology

Abstract

microRNAs regulate the development of myogenic progenitors, and the formation of skeletal muscle fibers. However, the role miRNAs play in controlling the growth and adaptation of post-mitotic musculature is less clear. Here, we show that inhibition of the established pro-myogenic regulator miR-206 can promote hypertrophy and increased protein synthesis in post-mitotic cells of the myogenic lineage. We have previously demonstrated that histone deacetylase 4 (HDAC4) is a target of miR-206 in the regulation of myogenic differentiation. We confirmed that inhibition of miR-206 de-repressed HDAC4 accumulation in cultured myotubes. Importantly, inhibition of HDAC4 activity by valproic acid or sodium butyrate prevented hypertrophy of myogenic cells otherwise induced by inhibition of miR-206. To test the significance of miRNA-206 as a regulator of skeletal muscle mass in vivo, we designed recombinant adeno-associated viral vectors (rAAV6 vectors) expressing miR-206, or a miR-206 "sponge," featuring repeats of a validated miR-206 target sequence. We observed that over-expression or inhibition of miR-206 in the muscles of mice decreased or increased endogenous HDAC4 levels respectively, but did not alter muscle mass or myofiber size. We subsequently manipulated miR-206 levels in muscles undergoing follistatin-induced hypertrophy or denervation-induced atrophy (models of muscle adaptation where endogenous miR-206 expression is altered). Vector-mediated manipulation of miR-206 activity in these models of cell growth and wasting did not alter gain or loss of muscle mass respectively. Our data demonstrate that although the miR-206/HDAC4 axis operates in skeletal muscle, the post-natal expression of miR-206 is not a key regulator of basal skeletal muscle mass or specific modes of muscle growth and wasting. These studies support a context-dependent role of miR-206 in regulating hypertrophy that may be dispensable for maintaining or modifying the adult skeletal muscle phenotype--an important consideration in relation to the development of therapeutics designed to manipulate microRNA activity in musculature.

Published

2013

12. Therapeutic inhibition of the miR-34 family attenuates pathological cardiac remodeling and improves heart function.

Author

Bernardo BC, Gao XM, Winbanks CE, Boey EJ, Tham YK, Kiriazis H, Gregorevic P, Obad S, Kauppinen S, Du XJ, Lin RC, and McMullen JR

Subjects

Animals, Base Sequence, DNA, DNA-Binding Proteins metabolism, Fucosyltransferases metabolism, Mice, Molecular Sequence Data, Neovascularization, Pathologic, Oligonucleotides chemistry, Proto-Oncogene Proteins c-bcl-6, Semaphorins metabolism, Up-Regulation, Vinculin metabolism, Heart Function Tests, MicroRNAs antagonists & inhibitors, Ventricular Remodeling

Abstract

MicroRNAs are dysregulated in a setting of heart disease and have emerged as promising therapeutic targets. MicroRNA-34 family members (miR-34a, -34b, and -34c) are up-regulated in the heart in response to stress. In this study, we assessed whether inhibition of the miR-34 family using an s.c.-delivered seed-targeting 8-mer locked nucleic acid (LNA)-modified antimiR (LNA-antimiR-34) can provide therapeutic benefit in mice with preexisting pathological cardiac remodeling and dysfunction due to myocardial infarction (MI) or pressure overload via transverse aortic constriction (TAC). An additional cohort of mice subjected to MI was given LNA-antimiR-34a (15-mer) to inhibit miR-34a alone as a comparison for LNA-antimiR-34. LNA-antimiR-34 (8-mer) efficiently silenced all three miR-34 family members in both cardiac stress models and attenuated cardiac remodeling and atrial enlargement. In contrast, inhibition of miR-34a alone with LNA-antimiR-34a (15-mer) provided no benefit in the MI model. In mice subjected to pressure overload, LNA-antimiR-34 improved systolic function and attenuated lung congestion, associated with reduced cardiac fibrosis, increased angiogenesis, increased Akt activity, decreased atrial natriuretic peptide gene expression, and maintenance of sarcoplasmic reticulum Ca(2+) ATPase gene expression. Improved outcome in LNA-antimiR-34-treated MI and TAC mice was accompanied by up-regulation of several direct miR-34 targets, including vascular endothelial growth factors, vinculin, protein O-fucosyltranferase 1, Notch1, and semaphorin 4B. Our results provide evidence that silencing of the entire miR-34 family can protect the heart against pathological cardiac remodeling and improve function. Furthermore, these data underscore the utility of seed-targeting 8-mer LNA-antimiRs in the development of new therapeutic approaches for pharmacologic inhibition of disease-implicated miRNA seed families.

Published

2012

13. Follistatin-mediated skeletal muscle hypertrophy is regulated by Smad3 and mTOR independently of myostatin.

Author

Winbanks CE, Weeks KL, Thomson RE, Sepulveda PV, Beyer C, Qian H, Chen JL, Allen JM, Lancaster GI, Febbraio MA, Harrison CA, McMullen JR, Chamberlain JS, and Gregorevic P

Subjects

Animals, Follistatin genetics, HEK293 Cells, Humans, Hypertrophy metabolism, Mice, Mice, Inbred C57BL, Myostatin genetics, Signal Transduction, Follistatin metabolism, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Myostatin metabolism, Smad3 Protein metabolism, TOR Serine-Threonine Kinases metabolism

Abstract

Follistatin is essential for skeletal muscle development and growth, but the intracellular signaling networks that regulate follistatin-mediated effects are not well defined. We show here that the administration of an adeno-associated viral vector expressing follistatin-288aa (rAAV6:Fst-288) markedly increased muscle mass and force-producing capacity concomitant with increased protein synthesis and mammalian target of rapamycin (mTOR) activation. These effects were attenuated by inhibition of mTOR or deletion of S6K1/2. Furthermore, we identify Smad3 as the critical intracellular link that mediates the effects of follistatin on mTOR signaling. Expression of constitutively active Smad3 not only markedly prevented skeletal muscle growth induced by follistatin but also potently suppressed follistatin-induced Akt/mTOR/S6K signaling. Importantly, the regulation of Smad3- and mTOR-dependent events by follistatin occurred independently of overexpression or knockout of myostatin, a key repressor of muscle development that can regulate Smad3 and mTOR signaling and that is itself inhibited by follistatin. These findings identify a critical role of Smad3/Akt/mTOR/S6K/S6RP signaling in follistatin-mediated muscle growth that operates independently of myostatin-driven mechanisms.

Published

2012

14. Suppression of microRNA-29 expression by TGF-β1 promotes collagen expression and renal fibrosis.

Author

Wang B, Komers R, Carew R, Winbanks CE, Xu B, Herman-Edelstein M, Koh P, Thomas M, Jandeleit-Dahm K, Gregorevic P, Cooper ME, and Kantharidis P

Subjects

3' Untranslated Regions genetics, Animals, Cadherins genetics, Cells, Cultured, Diabetic Nephropathies metabolism, Fibrosis, Gene Expression Regulation, Kidney metabolism, Male, Mice, Mice, Inbred BALB C, RNA, Messenger analysis, Rats, Rats, Sprague-Dawley, Transforming Growth Factor beta1 pharmacology, Collagen genetics, Kidney pathology, MicroRNAs physiology

Abstract

Synthesis and deposition of extracellular matrix (ECM) within the glomerulus and interstitium characterizes renal fibrosis, but the mechanisms underlying this process are incompletely understood. The profibrotic cytokine TGF-β1 modulates the expression of certain microRNAs (miRNAs), suggesting that miRNAs may have a role in the pathogenesis of renal fibrosis. Here, we exposed proximal tubular cells, primary mesangial cells, and podocytes to TGF-β1 to examine its effect on miRNAs and subsequent collagen synthesis. TGF-β1 reduced expression of the miR-29a/b/c/family, which targets collagen gene expression, and increased expression of ECM proteins. In both resting and TGF-β1-treated cells, ectopic expression of miR-29 repressed the expression of collagens I and IV at both the mRNA and protein levels by targeting the 3'untranslated region of these genes. Furthermore, we observed low levels of miR-29 in three models of renal fibrosis representing early and advanced stages of disease. Administration of the Rho-associated kinase inhibitor fasudil prevented renal fibrosis and restored expression of miR-29. Taken together, these data suggest that TGF-β1 inhibits expression of the miR-29 family, thereby promoting expression of ECM components. Pharmacologic modulation of these miRNAs may have therapeutic potential for progressive renal fibrosis.

Published

2012

15. Transduction of skeletal muscles with common reporter genes can promote muscle fiber degeneration and inflammation.

Author

Winbanks CE, Beyer C, Qian H, and Gregorevic P

Subjects

Alkaline Phosphatase administration & dosage, Alkaline Phosphatase genetics, Animals, Cytomegalovirus genetics, Dependovirus genetics, GPI-Linked Proteins administration & dosage, GPI-Linked Proteins genetics, Genetic Vectors administration & dosage, Genetic Vectors genetics, Green Fluorescent Proteins metabolism, HEK293 Cells, Humans, Injections, Intramuscular, Isoenzymes administration & dosage, Isoenzymes genetics, Macrophages metabolism, Male, Mice, Mice, Inbred C57BL, Organ Specificity genetics, Promoter Regions, Genetic genetics, Signal Transduction, T-Lymphocytes metabolism, Time Factors, Genes, Reporter genetics, Inflammation pathology, Muscle Fibers, Skeletal metabolism, Muscle Fibers, Skeletal pathology, Transduction, Genetic

Abstract

Recombinant adeno-associated viral vectors (rAAV vectors) are promising tools for delivering transgenes to skeletal muscle, in order to study the mechanisms that control the muscle phenotype, and to ameliorate diseases that perturb muscle homeostasis. Many studies have employed rAAV vectors carrying reporter genes encoding for β-galactosidase (β-gal), human placental alkaline phosphatase (hPLAP), and green fluorescent protein (GFP) as experimental controls when studying the effects of manipulating other genes. However, it is not clear to what extent these reporter genes can influence signaling and gene expression signatures in skeletal muscle, which may confound the interpretation of results obtained in experimentally manipulated muscles. Herein, we report a strong pro-inflammatory effect of expressing reporter genes in skeletal muscle. Specifically, we show that the administration of rAAV6:hPLAP vectors to the hind limb muscles of mice is associated with dose- and time-dependent macrophage recruitment, and skeletal muscle damage. Dose-dependent expression of hPLAP also led to marked activity of established pro-inflammatory IL-6/Stat3, TNFα, IKKβ and JNK signaling in lysates obtained from homogenized muscles. These effects were independent of promoter type, as expression cassettes featuring hPLAP under the control of constitutive CMV and muscle-specific CK6 promoters both drove cellular responses when matched for vector dose. Importantly, the administration of rAAV6:GFP vectors did not induce muscle damage or inflammation except at the highest doses we examined, and administration of a transgene-null vector (rAAV6:MCS) did not cause damage or inflammation at any of the doses tested, demonstrating that GFP-expressing, or transgene-null vectors may be more suitable as experimental controls. The studies highlight the importance of considering the potential effects of reporter genes when designing experiments that examine gene manipulation in vivo.

Published

2012

16. TGF-beta regulates miR-206 and miR-29 to control myogenic differentiation through regulation of HDAC4.

Author

Winbanks CE, Wang B, Beyer C, Koh P, White L, Kantharidis P, and Gregorevic P

Subjects

3' Untranslated Regions, Animals, Cell Differentiation, Cell Line, Gene Expression Regulation, Humans, Mice, Muscle Development, Muscles pathology, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction, Histone Deacetylases metabolism, MicroRNAs metabolism, Transforming Growth Factor beta metabolism

Abstract

MicroRNAs (miRs) are emerging as prominent players in the regulation of many biological processes, including myogenic commitment and skeletal muscle formation. Members of the TGF-β family can influence the proliferation and myogenic differentiation of cells, although it is presently not clear what role miRNAs play in the TGF-β-mediated control of myogenic differentiation. Here, we demonstrate in the myogenic C2C12 cell line, and in primary muscle cells, that miR-206 and miR-29-two miRs that act on transcriptional events implicated in muscle differentiation are down-regulated by TGF-β. We further demonstrate that TGF-β treatment of myogenic cells is associated with increased expression of histone deacetylase 4 (HDAC4), a key inhibitor of muscle differentiation that has been identified as a target for regulation by miR-206 and miR-29. We confirmed that increased expression of miR-206 and miR-29 resulted in the translational repression of HDAC4 in the presence or absence of TGF-β via interaction with the HDAC4 3'-untranslated region. Importantly, we found that miR-206 and miR-29 can attenuate the inhibitory actions of TGF-β on myogenic differentiation. Furthermore, we present evidence that the mechanism by which miR-206 and miR-29 can inhibit the TGF-β-mediated up-regulation of HDAC4 is via the inhibition of Smad3 expression, a transducer of TGF-β signaling. These findings identify a novel mechanism of interaction between TGF-β and miR-206 and -29 in the regulation of myogenic differentiation through HDAC4.

Published

2011

17. Explanting is an ex vivo model of renal epithelial-mesenchymal transition.

Author

Winbanks CE, Darby IA, Kelynack KJ, Pouniotis D, Becker GJ, and Hewitson TD

Subjects

Animals, Biomarkers analysis, Cell Culture Techniques, Cell Differentiation physiology, Cell Proliferation, Endothelial Cells cytology, Endothelial Cells metabolism, Epithelial Cells metabolism, Immunochemistry methods, Mesenchymal Stem Cells metabolism, Myofibroblasts metabolism, Phenotype, Rats, Rats, Sprague-Dawley, Staining and Labeling methods, Epithelial Cells cytology, Epithelial-Mesenchymal Transition physiology, Kidney cytology, Kidney Tubules, Proximal metabolism, Mesenchymal Stem Cells cytology, Myofibroblasts cytology

Abstract

Recognised by their de novo expression of alpha-smooth muscle actin (SMA), recruitment of myofibroblasts is key to the pathogenesis of fibrosis in chronic kidney disease. Increasingly, we realise that epithelial-mesenchymal transition (EMT) may be an important source of these cells. In this study we describe a novel model of renal EMT. Rat kidney explants were finely diced on gelatin-coated Petri dishes and cultured in serum-supplemented media. Morphology and immunocytochemistry were used to identify mesenchymal (vimentin+, α-smooth muscle actin (SMA)+, desmin+), epithelial (cytokeratin+), and endothelial (RECA+) cells at various time points. Cell outgrowths were all epithelial in origin (cytokeratin+) at day 3. By day 10, 50 ± 12% (mean ± SE) of cytokeratin+ cells double-labelled for SMA, indicating EMT. Lectin staining established a proximal tubule origin. By day 17, cultures consisted only of myofibroblasts (SMA+/cytokeratin-). Explanting is a reproducible ex vivo model of EMT. The ability to modify this change in phenotype provides a useful tool to study the regulation and mechanisms of renal tubulointerstitial fibrosis.

Published

2011

18. Genetic dissection of differential signaling threshold requirements for the Wnt/beta-catenin pathway in vivo.

Author

Buchert M, Athineos D, Abud HE, Burke ZD, Faux MC, Samuel MS, Jarnicki AG, Winbanks CE, Newton IP, Meniel VS, Suzuki H, Stacker SA, Näthke IS, Tosh D, Huelsken J, Clarke AR, Heath JK, Sansom OJ, and Ernst M

Subjects

Adenomatous Polyposis Coli Protein genetics, Adenomatous Polyposis Coli Protein metabolism, Animals, Cells, Cultured, Embryo, Mammalian, Female, Fibroblasts metabolism, Intestinal Mucosa metabolism, Intestines embryology, Intestines growth & development, Liver embryology, Liver growth & development, Liver metabolism, Male, Mice embryology, Mice growth & development, Mice, Inbred C57BL, Mice, Knockout, Wnt Proteins, Wnt3 Protein, beta Catenin genetics, Mice genetics, Mice metabolism, Signal Transduction, beta Catenin metabolism

Abstract

Contributions of null and hypomorphic alleles of Apc in mice produce both developmental and pathophysiological phenotypes. To ascribe the resulting genotype-to-phenotype relationship unambiguously to the Wnt/beta-catenin pathway, we challenged the allele combinations by genetically restricting intracellular beta-catenin expression in the corresponding compound mutant mice. Subsequent evaluation of the extent of resulting Tcf4-reporter activity in mouse embryo fibroblasts enabled genetic measurement of Wnt/beta-catenin signaling in the form of an allelic series of mouse mutants. Different permissive Wnt signaling thresholds appear to be required for the embryonic development of head structures, adult intestinal polyposis, hepatocellular carcinomas, liver zonation, and the development of natural killer cells. Furthermore, we identify a homozygous Apc allele combination with Wnt/beta-catenin signaling capacity similar to that in the germline of the Apc(min) mice, where somatic Apc loss-of-heterozygosity triggers intestinal polyposis, to distinguish whether co-morbidities in Apc(min) mice arise independently of intestinal tumorigenesis. Together, the present genotype-phenotype analysis suggests tissue-specific response levels for the Wnt/beta-catenin pathway that regulate both physiological and pathophysiological conditions., Competing Interests: The authors have declared that no competing interests exist.

Published

2010

19. Lectin histochemistry for light and electron microscopy.

Author

Wong SE, Winbanks CE, Samuel CS, and Hewitson TD

Subjects

Animals, Glycoconjugates chemistry, In Vitro Techniques, Paraffin Embedding, Rats, Histocytochemistry methods, Lectins chemistry, Microscopy methods, Microscopy, Electron methods

Abstract

Glycoconjugates are complex macromolecules present in all tissues throughout the body. Depending on the tissue region, glycoconjugates express different carbohydrate moieties, which can be used to both distinguish cell type and examine changes in cell phenotype.Although the periodic acid-schiff (PAS) method has long been used to study the distribution of glycoconjugates, the usefulness of the technique is severely limited by its lack of specificity. A more specific technique makes use of the affinity that plant-derived lectins have for different carbohydrate moieties in glycoconjugates. Binding of lectins is therefore a particularly useful adjunct to conventional histology when it is important to characterise cell type. These well-characterised binding patterns have proved particularly valuable in helping us understand the pathogenesis of kidney disease, changes in cell surface carbohydrates on normal and neoplastic cells in tumours, and blood group biology.When labeled with a reporter molecule such as biotin or gold, lectin binding can be easily identified using light and electron microscopy. In this chapter, we describe the appropriate experimental protocols for light and electron microscopic examination of lectin binding, emphasising their utility in characterising nephron segments in renal disease.

Published

2010

20. Role of the phosphatidylinositol 3-kinase and mTOR pathways in the regulation of renal fibroblast function and differentiation.

Author

Winbanks CE, Grimwood L, Gasser A, Darby IA, Hewitson TD, and Becker GJ

Subjects

Actins biosynthesis, Animals, Apoptosis drug effects, Cell Differentiation drug effects, Cell Proliferation drug effects, Cells, Cultured, Chromones pharmacology, Enzyme Inhibitors pharmacology, Fibroblasts cytology, Gene Expression Regulation drug effects, Kidney cytology, Morpholines pharmacology, Muscle Cells cytology, Muscle Cells enzymology, Phosphoinositide-3 Kinase Inhibitors, Rats, Signal Transduction drug effects, TOR Serine-Threonine Kinases, Cell Differentiation physiology, Fibroblasts enzymology, Kidney enzymology, Phosphatidylinositol 3-Kinases metabolism, Protein Kinases metabolism, Signal Transduction physiology

Abstract

Tubulointerstitial fibrosis is largely mediated by (myo)fibroblasts present in the interstitium. In this study, we investigated the role of mTOR and phosphatidylinositol 3-kinase in the regulation of fibroblast kinetics, fibroblast differentiation, and collagen synthesis. Rat renal fibroblasts were propagated from kidneys 3 days post-ureteric obstruction and specific inhibitors of mTOR (RAD) and phosphatidylinositol 3-kinase (LY294002) were used to examine the regulation of fibrogenesis. LY294002 but not RAD completely inhibited phosphorylation of Akt, while both inhibitors decreased phosphorylation of the S6 ribosomal protein. RAD and LY decreased foetal calf serum stimulated proliferation and DNA synthesis. In addition to their individual effects, treatment with both RAD and LY294002 decreased serum-induced fibroblast proliferation and DNA synthesis significantly more than either drug alone. TUNEL positive cells (apoptosis) in RAD and LY294002 treated groups were not different from control groups. In addition to their effect on proliferation, both inhibitors also reduced total collagen synthesis. Differentiation studies indicated an increase in alpha-smooth muscle actin expression relative to beta-actin (western blotting), with cytochemistry confirming that all doses of RAD and LY294002 increased the proportion of alpha-smooth muscle actin positive cells, and hence myofibroblasts. Effects were independent of cell toxicity. These results highlight the potential significance of PI3K and mTOR, in the regulation of renal (myo)fibroblast activity. The synergistic effects of LY and RAD on proliferation suggest that mTOR signalling involves pathways other than phosphatidylinositol 3-kinase. These results provide a novel insight into the mechanisms of fibroblast regulation during fibrogenesis.

Published

2007