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19 results on '"Sorci, Guglielmo"'

1. S100B engages RAGE or bFGF/FGFR1 in myoblasts depending on its own concentration and myoblast density. Implications for muscle regeneration.

Author

Riuzzi F, Sorci G, Beccafico S, and Donato R

Subjects
Animals, Blotting, Western, Cattle, Cell Differentiation genetics, Cell Differentiation physiology, Cell Line, Cell Proliferation, Cells, Cultured, Fibroblast Growth Factor 2 genetics, Immunohistochemistry, Immunoprecipitation, Mice, Mice, Inbred C57BL, Mice, Knockout, Mitogen-Activated Protein Kinase 1 genetics, Mitogen-Activated Protein Kinase 1 metabolism, Mitogen-Activated Protein Kinase 3 genetics, Mitogen-Activated Protein Kinase 3 metabolism, Muscle, Skeletal cytology, Myoblasts cytology, Protein Binding, Receptor for Advanced Glycation End Products, Receptor, Fibroblast Growth Factor, Type 1 genetics, Receptors, Immunologic genetics, Reverse Transcriptase Polymerase Chain Reaction, S100 Proteins genetics, p38 Mitogen-Activated Protein Kinases genetics, p38 Mitogen-Activated Protein Kinases metabolism, Fibroblast Growth Factor 2 metabolism, Muscle, Skeletal metabolism, Myoblasts metabolism, Receptor, Fibroblast Growth Factor, Type 1 metabolism, Receptors, Immunologic metabolism, Regeneration physiology, S100 Proteins metabolism
Abstract

In high-density myoblast cultures S100B enhances basic fibroblast growth factor (bFGF) receptor 1 (FGFR1) signaling via binding to bFGF and blocks its canonical receptor, receptor for advanced glycation end-products (RAGE), thereby stimulating proliferation and inhibiting differentiation. Here we show that upon skeletal muscle injury S100B is released from myofibers with maximum release at day 1 post-injury in coincidence with satellite cell activation and the beginning of the myoblast proliferation phase, and declining release thereafter in coincidence with reduced myoblast proliferation and enhanced differentiation. By contrast, levels of released bFGF are remarkably low at day 1 post-injury, peak around day 5 and decline thereafter. We also show that in low-density myoblast cultures S100B binds RAGE, but not bFGF/FGFR1 thereby simultaneously stimulating proliferation via ERK1/2 and activating the myogenic program via p38 MAPK. Clearance of S100B after a 24-h treatment of low-density myoblasts results in enhanced myotube formation compared with controls as a result of increased cell numbers and activated myogenic program, whereas chronic treatment with S100B results in stimulation of proliferation and inhibition of differentiation due to a switch of the initial low-density culture to a high-density culture. However, at relatively high doses, S100B stimulates the mitogenic bFGF/FGFR1 signaling in low-density myoblasts, provided bFGF is present. We propose that S100B is a danger signal released from injured muscles that participates in skeletal muscle regeneration by activating the promyogenic RAGE or the mitogenic bFGF/FGFR1 depending on its own concentration, the absence or presence of bFGF, and myoblast density.

Published
2012
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2. S100B protein regulates myoblast proliferation and differentiation by activating FGFR1 in a bFGF-dependent manner.

Author

Riuzzi F, Sorci G, and Donato R

Subjects
Animals, Cell Differentiation physiology, Cell Growth Processes physiology, Cell Line, Humans, Mice, Mice, Inbred C57BL, Phosphorylation, Receptor for Advanced Glycation End Products, Receptors, Immunologic metabolism, S100 Calcium Binding Protein beta Subunit, Signal Transduction, Up-Regulation, Fibroblast Growth Factor 2 metabolism, Myoblasts cytology, Myoblasts metabolism, Nerve Growth Factors metabolism, Receptor, Fibroblast Growth Factor, Type 1 metabolism, S100 Proteins metabolism
Abstract

S100B protein has been shown to exert anti-myogenic and mitogenic effects in myoblast cultures through inhibition of the myogenic p38 MAPK and activation of the mitogenic ERK1/2. However, the receptor mediating these effects had not been identified. Here, we show that S100B increases and/or stabilizes the binding of basic fibroblast growth factor (bFGF) to bFGF receptor 1 (FGFR1) by interacting with bFGF, thereby enhancing FGFR1 activation and the mitogenic and anti-myogenic effects of FGFR1. S100B also binds to its canonical receptor RAGE (receptor for advanced glycation end-products), a multi-ligand receptor previously shown to transduce a pro-myogenic signal when activated by HMGB1, and recruits RAGE into a RAGE-S100B-bFGF-FGFR1 complex. However, when bound to S100B-bFGF-FGFR1, RAGE can no longer stimulate myogenic differentiation, whereas in the absence of either bFGF or FGFR1, binding of S100B to RAGE results in stimulation of RAGE anti-mitogenic and promyogenic signaling. An S100B-bFGF-FGFR1 complex also forms in Rage(-/-) myoblasts, leading to enhanced proliferation and reduced differentiation, which points to a dispensability of RAGE for the inhibitory effects of S100B on myoblasts under the present experimental conditions. These results reveal a new S100B-interacting protein - bFGF - in the extracellular milieu and suggest that S100B stimulates myoblast proliferation and inhibits myogenic differentiation by activating FGFR1 in a bFGF-dependent manner.

Published
2011
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3. S100B stimulates myoblast proliferation and inhibits myoblast differentiation by independently stimulating ERK1/2 and inhibiting p38 MAPK.

Author

Riuzzi F, Sorci G, and Donato R

Subjects
Animals, Antioxidants pharmacology, Apoptosis drug effects, Cell Cycle drug effects, Creatine Kinase, MM Form metabolism, Cyclin D1 metabolism, Cyclin-Dependent Kinase Inhibitor p21 metabolism, Dose-Response Relationship, Drug, Mitogen-Activated Protein Kinase 1 metabolism, Mitogen-Activated Protein Kinase 3 metabolism, Myoblasts cytology, Myoblasts metabolism, NF-kappa B antagonists & inhibitors, NF-kappa B metabolism, Phosphorylation drug effects, Protein Kinase Inhibitors pharmacology, Rats, Retinoblastoma Protein metabolism, S100 Calcium Binding Protein beta Subunit, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors, ras Proteins metabolism, Cell Differentiation drug effects, Cell Proliferation drug effects, Mitogen-Activated Protein Kinases metabolism, Myoblasts drug effects, Nerve Growth Factors pharmacology, S100 Proteins pharmacology, p38 Mitogen-Activated Protein Kinases metabolism
Abstract

The Ca2+-modulated protein of the EF-hand type, S100B, was shown to inhibit rat L6 myoblast differentiation and myotube formation by interacting with a high affinity with an unidentified receptor (Sorci et al., 2003). We show here that S100B independently inhibits the MKK6-p38 MAPK pathway and stimulates the Ras-MEK-ERK1/2 pathway. The inhibitory effect of S100B on p38 MAPK translates into a defective induction of the muscle-specific transcription factor myogenin and the antiproliferative factor p21(WAF1), while S100B's stimulatory effect on ERK1/2 results in stimulation of myoblast proliferation via cyclin D1 induction and Rb phosphorylation and protection against apoptosis via activation of NF-kappaB transcriptional activity. Also, the S100B's effects that are mediated by the Ras-MEK-ERK1/2 pathway that is, stimulation of proliferation and protection against apoptosis, depend on reactive oxygen species production, being inhibited by antioxidants, while the S100B inhibitory effect on the MKK6-p38 MAPK pathway is not. We propose that S100B might participate in the regulation of myoblast differentiation by stimulating myoblast proliferation, protecting myoblasts against apoptosis, and modulating myotube formation.

Published
2006
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4. The amphoterin (HMGB1)/receptor for advanced glycation end products (RAGE) pair modulates myoblast proliferation, apoptosis, adhesiveness, migration, and invasiveness. Functional inactivation of RAGE in L6 myoblasts results in tumor formation in vivo.

Author

Riuzzi F, Sorci G, and Donato R

Subjects
Actins metabolism, Animals, Apoptosis, Blotting, Western, Caveolin 3 metabolism, Cell Adhesion, Cell Differentiation, Cell Line, Cell Movement, Cell Proliferation, Cell Transformation, Neoplastic, Cells, Cultured, Gene Expression Regulation, Integrin beta1 metabolism, Ligands, Luciferases metabolism, MAP Kinase Signaling System, Mice, Mice, SCID, Mitogen-Activated Protein Kinase 1 metabolism, Mitogen-Activated Protein Kinase 3 metabolism, Mitogen-Activated Protein Kinases metabolism, Muscles metabolism, Neoplasm Invasiveness, Neoplasm Metastasis, Phosphorylation, Rats, Receptor for Advanced Glycation End Products, Time Factors, Transfection, p38 Mitogen-Activated Protein Kinases metabolism, Glycation End Products, Advanced metabolism, HMGB1 Protein metabolism, Myoblasts metabolism, Neoplasms metabolism, Receptors, Immunologic metabolism
Abstract

We reported that RAGE (receptor for advanced glycation end products), a multiligand receptor of the immunoglobulin superfamily expressed in myoblasts, when activated by its ligand amphoterin (HMGB1), stimulates rat L6 myoblast differentiation via a Cdc42-Rac-MKK6-p38 mitogen-activated protein kinase pathway, and that RAGE expression in skeletal muscle tissue is developmentally regulated. We show here that inhibition of RAGE function via overexpression of a signaling deficient RAGE mutant (RAGE delta cyto) results in increased myoblast proliferation, migration, and invasiveness, and decreased apoptosis and adhesiveness, whereas myoblasts overexpressing RAGE behave the opposite, compared with mock-transfected myoblasts. These effects are accompanied by a decreased induction of the proliferation inhibitor, p21(Waf1), and increased induction of cyclin D1 and extent of Rb, ERK1/2, and JNK phosphorylation in L6/RAGE delta cyto myoblasts, the opposite occurring in L6/RAGE myoblasts. Neutralization of culture medium amphoterin negates effects of RAGE activation, suggesting that amphoterin is the RAGE ligand involved in RAGE-dependent effects in myoblasts. Finally, mice injected with L6/RAGE delta cyto myoblasts develop tumors as opposed to mice injected with L6/RAGE or L6/mock myoblasts that do not. Thus, the amphoterin/RAGE pair stimulates myoblast differentiation by the combined effect of stimulation of differentiation and inhibition of proliferation, and deregulation of RAGE expression in myoblasts might contribute to their neoplastic transformation.

Published
2006
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5. S100B causes apoptosis in a myoblast cell line in a RAGE-independent manner.

Author

Sorci G, Riuzzi F, Agneletti AL, Marchetti C, and Donato R

Subjects
Animals, Apoptosis physiology, Blotting, Western, Cell Line, Electrophoresis, Polyacrylamide Gel, Glycation End Products, Advanced, Immunohistochemistry, Myoblasts metabolism, Rats, Receptor for Advanced Glycation End Products, S100 Calcium Binding Protein beta Subunit, Transfection, Apoptosis drug effects, Myoblasts drug effects, Nerve Growth Factors pharmacology, Receptors, Immunologic metabolism, S100 Proteins pharmacology
Abstract

S100B, a Ca(2+)-modulated protein with both intracellular and extracellular regulatory roles, is most abundant in astrocytes, is expressed in various amounts in several non-nervous cells and is also found in normal serum. Astrocytes secrete S100B, and extracellular S100B exerts trophic and toxic effects on neurons depending on its concentration, in part by interacting with the receptor for advanced glycation end products (RAGE). The presence of S100B in normal serum and elevation of its serum concentration in several non-nervous pathological conditions suggest that S100B-expressing cells outside the brain might release the protein and S100B might affect non-nervous cells. Recently we reported that at picomolar to nanomolar doses S100B inhibits rat L6 myoblast differentiation via inactivation of p38 kinase in a RAGE-independent manner. We show here that at >or=5 nM in the absence of and at >100 nM in the presence of serum S100B causes myoblast apoptosis via stimulation of reactive oxygen species (ROS) production and inhibition of the pro-survival kinase, extracellular signal-regulated kinase (ERK)1/2, again in a RAGE-independent manner. Together with our previous data, the present results suggest that S100B might participate in the regulation of muscle development and regeneration by two independent mechanism, i.e., by inhibiting crucial steps of the myogenic program at the physiological levels found in serum and by causing elevation of ROS production and myoblast apoptosis following accumulation in serum and/or muscle extracellular space. Our data also suggest that RAGE has no role in the transduction of S100B effects on myoblasts, implying that S100B can interact with more than one receptor to affect its target cells.

Published
2004
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7. S100B protein regulates myoblast and macrophage functions in skeletal muscle regeneration

Author

Riuzzi, Francesca, Beccafico, Sara, Sagheddu, Roberta, Chiappalupi, Sara, Giambanco, Ileana, Sorci, Guglielmo, and Donato, Rosario

Subjects
Muscle regeneration, S100B, RAGE, bFGF/FGFR1, myoblasts, macrophages
Abstract

Regeneration of acutely injured skeletal muscles relies on a tightly controlled chain of cellular and molecular events, but a complete picture of factors concurring to the regeneration process is still missing. Extracellular S100B protein inhibits myoblast differentiation and stimulates myoblast proliferation by activating its canonical receptor, RAGE (receptor for advanced glycation endproducts), or bFGF/FGFR1 depending on myoblast density (1-4). S100B is released by damaged muscle tissue early after injury in advance of bFGF release, with declining release thereafter (4). We show that S100B is required for correct timing of skeletal muscle regeneration after acute injury. S100B expands the myoblast population, attracts macrophages to damage sites, promotes macrophage polarization into M2 (pro-regenerative) phenotype and reduces fibroblast proliferation. Also, S100B is transiently induced in and released by infiltrating macrophages under the action of proinflammatory and antiinflammatory cytokines, and effects of macrophage-derived S100B sum up with those of myofiber-released S100B. S100B’s effects are mediated by RAGE during the first 3 days after injury, however during the myoblast proliferation phase/macrophage M2 phase (i.e. at days 4-6 post-injury) S100B also activates bFGF-FGFR1 to stimulate myoblast proliferation and macrophage M1/M2 transition. Thus, S100B is a major molecular determinant of timed muscle regeneration after acute injury by virtue of its regulatory effects on myoblasts and macrophages.This work was supported by grants from MIUR PRIN-2010R8JK2X_004, AFM-Téléthon 16260 and Fondazione CRP 2012.0241.021., Italian Journal of Anatomy and Embryology, Vol. 121, No. 1 (Supplement) 2016

Published
2016

14. RAGE signaling deficiency in rhabdomyosarcoma cells causes upregulation of PAX7 and uncontrolled proliferation.

Author

Riuzzi, Francesca, Sorci, Guglielmo, Sagheddu, Roberta, Sidoni, Angelo, Alaggio, Rita, Ninfo, Vito, and Donato, Rosario

Subjects
*ADVANCED glycation end-products, *CELLULAR signal transduction, *RHABDOMYOSARCOMA, *CELL proliferation, *MYOBLASTS, *GENE expression
Abstract

Embryonal rhabdomyosarcomas (ERMSs) show elevated levels of PAX7, a transcription factor that marks quiescent adult muscle stem (satellite) cells and is important for proliferation and survival of activated satellite cells and whose timely repression is required for myogenic differentiation. However, the mechanism of PAX7 accumulation in ERMSs and whether high PAX7 causes uncontrolled proliferation in ERMS remains to be elucidated. The receptor for advanced glycation end-products (RAGE, encoded by AGER) transduces a myogenic and anti-proliferative signal in myoblasts, and stable transfection of the ERMS cell line TE671, which does not express RAGE, with AGER results in reduced proliferation and formation of tumor masses in vivo, and enhanced apoptosis and myogenic differentiation. Herein, we show that RAGE expression is low or absent in human ERMSs. We also show that in ERMS cells (1) PAX7 accumulates owing to absent or low RAGE signaling; (2) elevated PAX7 levels reduce RAGE expression and levels of MyoD and myogenin, muscle-specific transcription factors required for myoblast proliferation arrest and differentiation, respectively; (3) PAX7 supports myoblast proliferation by reducing the levels of MyoD, primarily by promoting its degradation; and (4), when ectopically expressed in ERMS cells, that RAGE upregulates myogenin which upregulates MyoD and downregulates PAX7, with consequent inhibition of proliferation and stimulation of differentiation. Thus, failure to express RAGE and, hence, MyoD and myogenin above a critical level in ERMS cells might result in deregulated PAX7 expression leading to uncontrolled proliferation and, potentially, to rhabdomyosarcomagenesis. [ABSTRACT FROM AUTHOR]

Published
2014
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15. HMGB1-RAGE regulates muscle satellite cell homeostasis through p38-MAPK- and myogenindependent repression of Pax7 transcription.

Author

Riuzzi, Francesca, Sorci, Guglielmo, Sagheddu, Roberta, and Donato, Rosario

Subjects
*MYOGENIN, *SATELLITE cells, *HOMEOSTASIS, *MYOBLASTS, *MUSCLE cells, *SKELETAL muscle
Abstract

Expression of the paired-box 7 (PAX7) transcription factor is regulated during both myoblast proliferation and differentiation: high levels of PAX7 compromise myogenic differentiation because of excess and prolonged proliferation, whereas low levels of PAX7 result in precocious differentiation. We showed that myogenin repressed Pax7 transcription in differentiating myoblasts by binding to specific recognition sites in the Pax7 promoter, and that high-mobility group box 1 (HMGB1)-receptor for advanced glycation end-products (RAGE) signaling was required for myogenin induction and myogenin-dependent repression of Pax7 transcription. In addition, PAX7 negatively and myogenin positively regulated RAGE expression. RAGE, a multiligand receptor of the immunoglobulin superfamily, was not expressed in adult skeletal muscles, and was transiently expressed in activated, proliferating and differentiating satellite cells (SCs) in injured muscles. Compared with wild-type muscles, Rage-/- muscles exhibited increased numbers of basal SCs that were further increased in injured Rage-/- muscles following elevated myoblast asymmetric division; complete regeneration of injured Rage-/- muscles was found to be delayed by ~1 week. Thus, RAGE signaling physiologically repressed Pax7 transcription in SCs by upregulating myogenin, thereby accelerating muscle regeneration and limiting SC self-renewal. [ABSTRACT FROM AUTHOR]

Published
2012
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16. Human muscle satellite cells show age-related differential expression of S100B protein and RAGE.

Author

Beccafico, Sara, Riuzzi, Francesca, Puglielli, Cristina, Mancinelli, Rosa, Fulle, Stefania, Sorci, Guglielmo, and Donato, Rosario

Subjects
AGING, MUSCLES, SATELLITE cells, MYOBLASTS, IMMUNOGLOBULINS
Abstract

During aging, skeletal muscles show reduced mass and functional capacity largely due to loss of the regenerative ability of satellite cells (SCs), the quiescent stem cells located beneath the basal lamina surrounding each myofiber. While both the external environment and intrinsic properties of SCs appear to contribute to the age-related SC deficiency, the latter ones have been poorly investigated especially in humans. In the present work, we analyzed several parameters of SCs derived from biopsies of vastus lateralis muscle from healthy non-trained young (28.7 ± 5.9 years; n = 10) and aged (77.3 ± 6.4 years; n = 11) people. Compared with young SCs, aged SCs showed impaired differentiation when cultured in differentiation medium, and exhibited the following: (1) reduced proliferation; (2) higher expression levels of S100B, a negative regulator of myoblast differentiation; (3) undetectable levels in growth medium of full-length RAGE (receptor for advanced glycation end products), a multiligand receptor of the immunoglobulin superfamily, the engagement of which enhances myoblast differentiation; and (4) lower expression levels of the transcription factors, MyoD and Pax7. Also, either overexpression of full-length RAGE or knockdown of S100B in aged SCs resulted in enhanced differentiation, while overexpression of either a non-transducing mutant of RAGE (RAGEΔcyto) or S100B in young SCs resulted in reduced differentiation compared with controls. Moreover, while aged SCs maintained the ability to respond to mitogenic factors (e.g., bFGF and S100B), they were no longer able to secrete these factors, unlike young SCs. These data support a role for intrinsic factors, besides the extracellular environment in the defective SC function in aged skeletal muscles. [ABSTRACT FROM AUTHOR]

Published
2011
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17. Sertoli cells have promyogenic and antifibrotic effects, and induce utrophin expression in human DMD myotubes with different mutations in a heregulin β1/ErbB2/ERK1/2-dependent manner.

Author

Chiappalupi, Sara, Salvadori, Laura, Arato, Iva, Mancuso, Francesca, Calvitti, Mario, Marchetti, Maria Cristina, Riuzzi, Francesca, Calafiore, Riccardo, Luca, Giovanni, and Sorci, Guglielmo

Subjects
SERTOLI cells, MYOBLASTS, DUCHENNE muscular dystrophy, GERM cells, DYSTROPHIN genes, SEMINIFEROUS tubules, FACIOSCAPULOHUMERAL muscular dystrophy
Abstract

Sertoli cells (SeC) are the major component of the seminiferous tubules, where they secrete a plethora of trophic and immunomodulatory factors necessary to development of germ cells [1]. For these characteristics, SeC have been widely used as a therapeutic approach in many pre-clinical studies, including Duchenne muscular dystrophy (DMD) [2,3]. DMD is a lethal, rare X-linked disease caused by mutation in the dystrophin gene (DMD). The absence of dystrophin compromises the integrity of the dystrophin glycoprotein complex (DGC) increasing susceptibility of sarcolemma to rupture during contraction, with consequent necrosis of myofibers and muscle chronic inflammation. In DMD patients, the contractile component of skeletal muscles is progressively replaced by adipose and fibrous tissues, compromising muscle functionality and leading to premature death [4]. Despite huge effort to find a cure, glucocorticoids remain the standard therapy for DMD patients, despite their limited efficacy and undesired side effects. We reported that a single intraperitoneal injection of microencapsulated porcine SeC translates into recovery of muscle morphology and performance in dystrophic mice. This was linked to the ability of SeC to restrain inflammation and upregulate the dystrophin paralogue, utrophin at the sarcolemma through the release of heregulin β1 [5,6]. Here, we report the direct effect of SeC on myoblasts/myotubes of murine origin or derived from healthy subjects and DMD patients with different mutations. We observed that SeC-secreted factors i) stimulate cell proliferation in the early phase of differentiation in C2C12, and human healthy and DMD myoblasts; ii) delay the expression of differentiation markers in the early phase, nevertheless stimulating terminal differentiation in DMD myoblasts; iii) restrain the fibrogenic phenotype in human fibroblasts, and inhibit myoblast-myofibroblast transdifferentiation in C2C12 cells treated with TGF-β, and in DMD myoblasts; iv) induce the upregulation of utrophin at the sarcolemma in DMD myotubes regardless of the mutation in a heregulin β1/ErbB2/ERK1/2-dependent manner, recruiting components of the DGC thus providing functional replacement of dystrophin. Altogether, these results further support the use of SeC as a potential treatment of DMD patients, and suggest that SeC might improve muscle regeneration, especially in the early phase when myoblasts have to proliferate to efficiently replace damaged myofibers. [ABSTRACT FROM AUTHOR]

Published
2021

18. Amphoterin Stimulates Myogenesis and Counteracts the Antimyogenic Factors Basic Fibroblast Growth Factor and S100B via RAGE Binding.

Author

Sorci, Guglielmo, Riuzzi, Francesca, Arcuri, Cataldo, Giambanco, Ileana, and Donato, Rosario

Subjects
*MYOGENESIS, *CELL receptors, *IMMUNOGLOBULINS, *INFLAMMATION, *CELL migration, *TUMOR growth, *MYOBLASTS, *FIBROBLASTS, *GROWTH factors
Abstract

The receptor for advanced glycation end products (RAGE), a multiligand receptor of the immunoglobulin superfamily, has been implicated in the inflammatory response, diabetic angiopathy and neuropathy, neurodegeneration, cell migration, tumor growth, neuroprotection, and neuronal differentiation. We show here that (i) RAGE is expressed in skeletal muscle tissue and its expression is developmentally regulated and (ii) RAGE engagement by amphoterin (HMGB1), a RAGE ligand, in rat L6 myoblasts results in stimulation of myogenic differentiation via activation of p38 mitogen-activated protein kinase (MAPK), up-regulation of myogenin and myosin heavy chain expression, and induction of muscle creatine kinase. No such effects were detected in myoblasts transfected with a RAGE mutant lacking the transducing domain or myoblasts transfected with a constitutively inactive form of the p38 MAPK upstream kinase, MAPK kinase 6, Cdc42, or Rac-1. Moreover, amphoterin counteracted the antimyogenic activity of the Ca2+-modulated protein S100B, which was reported to inhibit myogenic differentiation via inactivation of p38 MAPK, and basic fibroblast growth factor (bFGF), a known inhibitor of myogenic differentiation, in a manner that was inversely related to the S100B or bFGF concentration and directly related to the extent of RAGE expression. These data suggest that RAGE and amphoterin might play an important role in myogenesis, accelerating myogenic differentiation via Cdc42-Rac1-MAPK kinase 6-p38 MAPK. [ABSTRACT FROM AUTHOR]

Published
2004
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19. Sertoli Cells Improve Myogenic Differentiation, Reduce Fibrogenic Markers, and Induce Utrophin Expression in Human DMD Myoblasts.

Author

Salvadori, Laura, Chiappalupi, Sara, Arato, Iva, Mancuso, Francesca, Calvitti, Mario, Marchetti, Maria Cristina, Riuzzi, Francesca, Calafiore, Riccardo, Luca, Giovanni, and Sorci, Guglielmo

Subjects
SERTOLI cells, MYOBLASTS, DUCHENNE muscular dystrophy, FIBROBLASTS, MUSCLE regeneration, MUSCLE mass
Abstract

Duchenne muscular dystrophy (DMD) is an X-linked disease caused by mutations in DMD gene translating in lack of functional dystrophin and resulting in susceptibility of myofibers to rupture during contraction. Inflammation and fibrosis are critical hallmarks of DMD muscles, which undergo progressive degeneration leading to loss of independent ambulation in childhood and death by early adulthood. We reported that intraperitoneal injection of microencapsulated Sertoli cells (SeC) in dystrophic mice translates into recovery of muscle morphology and performance thanks to anti-inflammatory effects and induction of the dystrophin paralogue, utrophin at the muscle level, opening new avenues in the treatment of DMD. The aim of this study is to obtain information about the direct effects of SeC on myoblasts/myotubes, as a necessary step in view of a translational application of SeC-based approaches to DMD. We show that (i) SeC-derived factors stimulate cell proliferation in the early phase of differentiation in C2C12, and human healthy and DMD myoblasts; (ii) SeC delay the expression of differentiation markers in the early phase nevertheless stimulating terminal differentiation in DMD myoblasts; (iii) SeC restrain the fibrogenic potential of fibroblasts, and inhibit myoblast-myofibroblast transdifferentiation; and, (iv) SeC provide functional replacement of dystrophin in preformed DMD myotubes regardless of the mutation by inducing heregulin β1/ErbB2/ERK1/2-dependent utrophin expression. Altogether, these results show that SeC are endowed with promyogenic and antifibrotic effects on dystrophic myoblasts, further supporting their potential use in the treatment of DMD patients. Our data also suggest that SeC-based approaches might be useful in improving the early phase of muscle regeneration, during which myoblasts have to adequately proliferate to replace the damaged muscle mass. [ABSTRACT FROM AUTHOR]

Published
2021
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