1999
DOI: 10.1002/(sici)1097-4598(199906)22:6<724::aid-mus9>3.0.co;2-o
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Macrophages enhance muscle satellite cell proliferation and delay their differentiation

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Cited by 182 publications
(133 citation statements)
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“…Notably, macrophages secrete both signals such as TNF-a that worsen muscle wasting via activation of the FOXO transcription factor (66, 67) and molecules that have an opposite function, such as IGF-1, a central regulator of muscle regeneration (7,56,57), or IL-10 (59, 68, 69). The activation of distinct pathways in muscle cells depending on macrophage activation leading to growth or differentiation had been described and characterized in elegant earlier studies (12,(70)(71)(72)(73)(74)(75)(76)(77).…”
Section: Discussionmentioning
confidence: 99%
“…Notably, macrophages secrete both signals such as TNF-a that worsen muscle wasting via activation of the FOXO transcription factor (66, 67) and molecules that have an opposite function, such as IGF-1, a central regulator of muscle regeneration (7,56,57), or IL-10 (59, 68, 69). The activation of distinct pathways in muscle cells depending on macrophage activation leading to growth or differentiation had been described and characterized in elegant earlier studies (12,(70)(71)(72)(73)(74)(75)(76)(77).…”
Section: Discussionmentioning
confidence: 99%
“…At the population level, mpc growth depends on both cell-cycling activity and cell survival. Previous studies on mpc-supporting cues have focused on MP-released soluble growth factors (Robertson et al, 1993;Cantini and Carraro, 1995;Merly et al, 1999). Some particular growth factors, such as insulin growth factor I (IGF-I), in addition to being a potent myogenic differentiation factor (Tureckova et al, 2001), can both stimulate mpc proliferation in the presence of other soluble factors (Napier et al, 1999) and promote mpc survival (Lawlor and Rotwein, 2000).…”
Section: Discussionmentioning
confidence: 99%
“…However, other studies show differing results. The addition of macrophages to cultures of myogenic cells yielded increased proliferation of myogenic cells but reduced the expression of myogenin (69), suggesting that macrophage-derived products could inhibit muscle differentiation by affecting the transition from the proliferative stage to the early differentiation stage of myogenesis. Although the explanation for these reported differences in the effects of macrophages on myogenic cell differentiation have not been identified with certainty, part of the explanation may lie in unknown differences in the phenotype of the macrophages used in the assays.…”
Section: Changes In Myeloid Cell Phenotype In Muscle Following Injurymentioning
confidence: 99%