Nuclear Factor I-C Links Platelet-Derived Growth Factor and Transforming Growth Factor β1 Signaling to Skin Wound Healing Progression

Plasari, Genta; Calabrese, Alessandra; Dusserre, Yves; Gronostajski, Richard M.; McNair, Alan; Michalik, Liliane; Mermod, Nicolas

doi:10.1128/mcb.01921-08

Cited by 48 publications

(59 citation statements)

References 61 publications

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“…Our interpretation of a regulatory interplay between Nfix and cell cycle inhibitors, such as p21, is also supported by a previously described role of Nfix in the regulation of mitogenic pathways in other cell types (Nebl et al, 1994). Our conclusions are also in line with prior observations of regulatory relationships between TGF-b and other Nfi species (Plasari et al, 2009;Plasari et al, 2010) and of BMP7 and Matn2 (Ichikawa et al, 2008) to control the timing of skin-wound healing. In keeping with these findings, we observed severe wound-healing defects in Matn2 2/2 mice on a C57BL/6 genetic background (F. Deák and I.…”

Section: Research Articlesupporting

confidence: 81%

“…Nfi proteins have been implicated in the control of adult stem cells and tissue regeneration in connection with TGF-b signaling (Plasari et al, 2009;Plasari et al, 2010). Nfix has been shown to drive a transcriptional switch from embryonic to fetal myogenesis in vivo and in C2 culture by suppressing the effect of Nfia and activating fetal muscle genes (Messina et al, 2010).…”

Section: Matn2 Is Required For C2 Myoblast Differentiationmentioning

confidence: 99%

“…Accordingly, other members of the NFI family have been implicated in other regenerative processes of adult tissue in the context of TGF-b signaling. For instance, Nfic has been implicated in tooth morphogenesis, skin-wound healing and the onset of the follicle cycle leading to hair regeneration (Lee et al, 2009;Plasari et al, 2009;Plasari et al, 2010). An NFIC isoform was shown to harbor a TGF-b-responsive domain, and NFI-binding sites acting as TGF-b-responsive elements have been reported in several other ECM genes (Alevizopoulos et al, 1995;Alonso et al, 1996;Iozzo et al, 1997).…”

Section: Research Articlementioning

confidence: 99%

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Extracellular deposition of matrilin-2 controls the timing of the myogenic program during muscle regeneration

Deák¹,

Mátés²,

Korpos³

et al. 2014

Development

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BSTRACTHere, we identify a role for the matrilin-2 (Matn2) extracellular matrix protein in controlling the early stages of myogenic differentiation. We observed Matn2 deposition around proliferating, differentiating and fusing myoblasts in culture and during muscle regeneration in vivo. Silencing of Matn2 delayed the expression of the Cdk inhibitor p21 and of the myogenic genes Nfix, MyoD and Myog, explaining the retarded cell cycle exit and myoblast differentiation. Rescue of Matn2 expression restored differentiation and the expression of p21 and of the myogenic genes. TGF-b1 inhibited myogenic differentiation at least in part by repressing Matn2 expression, which inhibited the onset of a positive-feedback loop whereby Matn2 and Nfix activate the expression of one another and activate myoblast differentiation. In vivo, myoblast cell cycle arrest and muscle regeneration was delayed in Matn2 2/2 relative to wild-type mice. The expression levels of Trf3 and myogenic genes were robustly reduced in Matn2 2/2 fetal limbs and in differentiating primary myoblast cultures, establishing Matn2 as a key modulator of the regulatory cascade that initiates terminal myogenic differentiation. Our data thus identify Matn2 as a crucial component of a genetic switch that modulates the onset of tissue repair.

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Section: Research Articlesupporting

confidence: 81%

Section: Matn2 Is Required For C2 Myoblast Differentiationmentioning

confidence: 99%

Section: Research Articlementioning

confidence: 99%

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Extracellular deposition of matrilin-2 controls the timing of the myogenic program during muscle regeneration

Deák¹,

Mátés²,

Korpos³

et al. 2014

Development

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“…These abnormalities have been associated with a decreased proliferation of NFI-C-lacking dental cells due to the overexpression of transforming growth factor ␤1 (TGF-␤1) (8). In addition, we have also shown that NFI-C deficiency affects the normal progression of the skin wound healing process, which has been linked to altered platelet-derived growth factor (PDGF) and TGF-␤ signaling in the knockout animals (9).…”

mentioning

confidence: 81%

“…For instance, PDGF, a potent chemotactic agent for macrophages, is known to activate the growth of telogen follicles (49). We recently found that NFI-C is involved in the inflammatory phase of the skin healing process (9). The PDGF and TGF-␤1 pathways were both found to be affected by the lack of NFI-C, and the increased expressions of PDGF and its receptor ␣ chain were linked to an increased infiltration of macrophages in the skin wounds of knock-out mice.…”

Section: Discussionmentioning

confidence: 99%

Nuclear Factor I-C Regulates TGF-β-dependent Hair Follicle Cycling*

Plasari

Edelmann

Hogger

et al. 2010

Journal of Biological Chemistry

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Nuclear factor one transcription factors: Divergent functions in developmental versus adult stem cell populations

Harris

Genovesi

Gronostajski

et al. 2014

Developmental Dynamics

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Nuclear factor one (NFI) transcription factors are a group of site-specific DNA-binding proteins that are emerging as critical regulators of stem cell biology. During development NFIs promote the production of differentiated progeny at the expense of stem cell fate, with Nfi null mice exhibiting defects such as severely delayed brain and lung maturation, skeletomuscular defects and renal abnormalities, phenotypes that are often consistent with patients with congenital Nfi mutations. Intriguingly, recent research suggests that in adult tissues NFI factors play a qualitatively different role than during development, with NFIs serving to promote the survival and maintenance of slow-cycling adult stem cell populations rather than their differentiation. Here we review the role of NFI factors in development, largely focusing on their role as promoters of stem cell differentiation, and attempt to reconcile this with the emerging role of NFIs in adult stem cell niches.

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Nuclear Factor I-C Links Platelet-Derived Growth Factor and Transforming Growth Factor β1 Signaling to Skin Wound Healing Progression

Cited by 48 publications

References 61 publications

Extracellular deposition of matrilin-2 controls the timing of the myogenic program during muscle regeneration

Extracellular deposition of matrilin-2 controls the timing of the myogenic program during muscle regeneration

Nuclear Factor I-C Regulates TGF-β-dependent Hair Follicle Cycling*

Nuclear factor one transcription factors: Divergent functions in developmental versus adult stem cell populations

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