A Pax3/Pax7-dependent population of skeletal muscle progenitor cells

Relaix, Frédéric; Rocancourt, Didier; Mansouri, Ahmed; Buckingham, Margaret

doi:10.1038/nature03594

Cited by 984 publications

(1,089 citation statements)

References 23 publications

(19 reference statements)

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“…The mutant and transgenic animals and genotyping primers used in this work were published: Pax3 GFP , 5 Arx nlacZ , 13 Tg: 3F-nlacZ-2E, 37 MyoD À/À , 38 Myf5 GFPÀP , Myf5 loxP , Myf5 nlacZ . 7,39 In Tg:3F-nlacZ-2E mice, b-galactosidase expression is restricted to differentiated skeletal and cardiac muscle.…”

Section: Methodsmentioning

confidence: 99%

“…3 Embryonic, fetal myoblasts and satellite cells derive from a Pax3/Pax7-positive population of myogenic progenitors resident in the dermomyotome. 4,5 During skeletal muscle development these mesoderm-derived progenitors generate myoblasts, which become postmitotic and then terminally differentiate into multinucleated myotubes. The muscle regulatory factors (MRFs) MyoD, Myf5, Mrf4 and Myogenin 6 are key regulators of the myogenic program and when transfected in fibroblasts, can convert them to a myogenic fate.…”

mentioning

confidence: 99%

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The homeobox gene Arx is a novel positive regulator of embryonic myogenesis

Biressi

Messina²,

Collombat

et al. 2007

Cell Death Differ

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Skeletal muscle fibers form in overlapping, but distinct phases that depend on the generation of temporally different lineages of myogenic cells. During primary myogenesis (E10.5-E12.5 in the mouse), embryonic myoblasts fuse homotypically to generate primary fibers, whereas during later development (E14.5-E17.5), fetal myoblasts differentiate into secondary fibers. How these myogenic waves are regulated remains largely unknown. Studies have been hampered by the lack of markers which would distinguish embryonic from fetal myoblast populations. We show here that the homeobox gene Arx is strongly expressed in differentiating embryonic muscle, downstream of myogenic basic helix-loop-helix (bHLH) genes. Its expression progressively decreases during development. When overexpressed in the C2C12 myogenic cell line, Arx enhances differentiation. Accordingly, it stimulates the transcriptional activity from the Myogenin promoter and from multimerized E-boxes when co-expressed with MyoD and Mef2C in CH310T1/2. Furthermore, Arx co-immunoprecipitates with Mef2C, suggesting that it participates in the transcriptional regulatory network acting in embryonic muscle. Finally, embryonic myoblasts isolated from Arx-deficient embryos show a delayed differentiation in vivo together with an enhanced clonogenic capacity in vitro. We propose here that Arx acts as a novel positive regulator of embryonic myogenesis by synergizing with Mef2C and MyoD and by establishing an activating loop with Myogenin.

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Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 99%

The homeobox gene Arx is a novel positive regulator of embryonic myogenesis

Biressi

Messina²,

Collombat

et al. 2007

Cell Death Differ

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“…Recently, galectin-1 has been identified as a soluble factor present in myoblast-conditioned medium, that has the capacity to promote myogenic conversion of dermal fibroblasts [17] and fetal MSCs [15]. This conversion seems to occur via activation of the myogenic regulatory factors (MRFs), including Myf-5, MyoD, and myogenin [15], as observed during embryonic myogenesis [18][19][20]. Another reported approach [21] made use of activated Notch to generate skeletal muscle cells from human MSCs.…”

Section: E X P E R I M E N T a L C E L L R E S E A R Cmentioning

confidence: 99%

Pax3 activation promotes the differentiation of mesenchymal stem cells toward the myogenic lineage

Gang

Bosnakovski

Simsek

et al. 2008

Experimental Cell Research

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“…At the embryonic stage, PAX7 is first expressed in the central dermomyotome and then colocalized with PAX3 in the myotome (Relaix, Rocancourt, Mansouri & Buckingham, 2005). The PAX3 + /PAX7 + cells then become embryonic muscle progenitor cells, which enter into the myogenic process and are differentiated into myoblasts with the expression of MYF5 and MYOD (Bober et al., 1991; Rudnicki et al., 1993; Sassoon et al., 1989).…”

Section: Introductionmentioning

confidence: 99%

Synergistic effects of TGFβ2, WNT9a, and FGFR4 signals attenuate satellite cell differentiation during skeletal muscle development

Zhang

et al. 2018

Aging Cell

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SummarySatellite cells play a key role in the aging, generation, and damage repair of skeletal muscle. The molecular mechanism of satellite cells in these processes remains largely unknown. This study systematically investigated for the first time the characteristics of mouse satellite cells at ten different ages. Results indicated that the number and differentiation capacity of satellite cells decreased with age during skeletal muscle development. Transcriptome analysis revealed that 2,907 genes were differentially expressed at six time points at postnatal stage. WGCNA and GO analysis indicated that 1,739 of the 2,907 DEGs were mainly involved in skeletal muscle development processes. Moreover, the results of WGCNA and protein interaction analysis demonstrated that Tgfβ2, Wnt9a, and Fgfr4 were the key genes responsible for the differentiation of satellite cells. Functional analysis showed that TGFβ2 and WNT9a inhibited, whereas FGFR4 promoted the differentiation of satellite cells. Furthermore, each two of them had a regulatory relationship at the protein level. In vivo study also confirmed that TGFβ2 could regulate the regeneration of skeletal muscle, as well as the expression of WNT9a and FGFR4. Therefore, we concluded that the synergistic effects of TGFβ2, WNT9a, and FGFR4 were responsible for attenuating of the differentiation of aging satellite cells during skeletal muscle development. This study provided new insights into the molecular mechanism of satellite cell development. The target genes and signaling pathways investigated in this study would be useful for improving the muscle growth of livestock or treating muscle diseases in clinical settings.

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A Pax3/Pax7-dependent population of skeletal muscle progenitor cells

Cited by 984 publications

References 23 publications

The homeobox gene Arx is a novel positive regulator of embryonic myogenesis

The homeobox gene Arx is a novel positive regulator of embryonic myogenesis

Pax3 activation promotes the differentiation of mesenchymal stem cells toward the myogenic lineage

Synergistic effects of TGFβ2, WNT9a, and FGFR4 signals attenuate satellite cell differentiation during skeletal muscle development

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