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Pax3 regulation of FGF signaling affects the progression of embryonic progenitor cells into the myogenic program.Pax3对成纤维细胞生长因子(FGF)信号的调控影响胚胎祖细胞向生肌程序的进展。
Genes Dev. 2008 Jul 1;22(13):1828-37. doi: 10.1101/gad.477908.
3
The role of Pax genes in the development of tissues and organs: Pax3 and Pax7 regulate muscle progenitor cell functions.Pax基因在组织和器官发育中的作用:Pax3和Pax7调节肌肉祖细胞的功能。
Annu Rev Cell Dev Biol. 2007;23:645-73. doi: 10.1146/annurev.cellbio.23.090506.123438.
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Gas1 extends the range of Hedgehog action by facilitating its signaling.Gas1通过促进刺猬信号通路(Hedgehog signaling)来扩展其作用范围。
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Beta catenin-independent activation of MyoD in presomitic mesoderm requires PKC and depends on Pax3 transcriptional activity.前体中胚层中MyoD的β-连环蛋白非依赖性激活需要蛋白激酶C,并依赖于Pax3转录活性。
Dev Biol. 2007 Apr 15;304(2):604-14. doi: 10.1016/j.ydbio.2007.01.006. Epub 2007 Jan 9.
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Dev Biol. 2007 Feb 15;302(2):504-21. doi: 10.1016/j.ydbio.2006.10.009. Epub 2006 Oct 10.
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Hedgehog acts directly on the zebrafish dermomyotome to promote myogenic differentiation.刺猬因子直接作用于斑马鱼的皮肌节,以促进肌源性分化。
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9
A novel genetic hierarchy functions during hypaxial myogenesis: Pax3 directly activates Myf5 in muscle progenitor cells in the limb.一种新的基因调控层级在体轴下肌生成过程中发挥作用:Pax3直接激活肢体肌肉祖细胞中的Myf5。
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The Wnt/beta-catenin pathway regulates Gli-mediated Myf5 expression during somitogenesis.Wnt/β-连环蛋白信号通路在体节发生过程中调控Gli介导的Myf5表达。
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Shh的梯度建立了由Nkx3.2和Pax3诱导的相互抑制的体节细胞命运。

A gradient of Shh establishes mutually repressing somitic cell fates induced by Nkx3.2 and Pax3.

作者信息

Cairns Dana M, Sato Mie Elissa, Lee Philip G, Lassar Andrew B, Zeng Li

机构信息

Program in Cellular, Molecular and Developmental Biology, Sackler School of Graduate Biomedical Sciences, Tufts University, 136 Harrison Avenue, Boston, MA 02111, USA.

出版信息

Dev Biol. 2008 Nov 15;323(2):152-65. doi: 10.1016/j.ydbio.2008.08.024. Epub 2008 Sep 5.

DOI:10.1016/j.ydbio.2008.08.024
PMID:18796301
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3766898/
Abstract

Wnt and Sonic Hedgehog (Shh) signals are known to pattern the somite into dermomyotomal, myotomal and sclerotomal cell fates. By employing explants of presomitic mesoderm cultured with constant levels of Wnt3a conditioned medium and increasing levels of Shh, we found that differing levels of Shh signaling elicit differing responses from somitic cells: the lowest level of Shh signaling allows dermomyotomal gene expression, intermediate levels induce loss of dermomyotomal markers and activation of myogenic differentiation, and higher levels induce loss of myotomal markers and activation of sclerotomal gene expression. In addition, we have found that in the presence of high levels of Wnt signaling, instead of inducing sclerotomal markers, Shh signals act to maintain the expression of dermomyotomal and myotomal markers. One of the sclerotomal genes induced by high levels of Shh signaling is Nkx3.2. Forced expression of Nkx3.2 blocks somitic expression of the dermomyotomal marker Pax3 both in vitro and in vivo. Conversely, forced expression of Pax3 in somites can block Shh-mediated induction of sclerotomal gene expression and chondrocyte differentiation in vitro. Thus we propose that varying levels of Shh signaling act in a morphogen-like manner to elicit differing responses from somitic cells, and that Pax3 and Nkx3.2 set up mutually repressing cell fates that promote either dermomyotome/myotome or sclerotome differentiation, respectively.

摘要

已知Wnt和音猬因子(Shh)信号可将体节分化为皮肌节、肌节和骨节细胞命运。通过使用在前体中胚层外植体中培养恒定水平的Wnt3a条件培养基并增加Shh水平,我们发现不同水平的Shh信号会引起体节细胞的不同反应:最低水平的Shh信号允许皮肌节基因表达,中等水平诱导皮肌节标记物的丧失和肌源性分化的激活,而较高水平诱导肌节标记物的丧失和骨节基因表达的激活。此外,我们发现,在高水平Wnt信号存在的情况下,Shh信号不是诱导骨节标记物,而是起到维持皮肌节和肌节标记物表达的作用。高水平Shh信号诱导的骨节基因之一是Nkx3.2。Nkx3.2的强制表达在体外和体内均可阻断皮肌节标记物Pax3在体节中的表达。相反,在体节中强制表达Pax3可在体外阻断Shh介导的骨节基因表达诱导和软骨细胞分化。因此,我们提出,不同水平的Shh信号以形态发生素样的方式起作用,以引起体节细胞的不同反应,并且Pax3和Nkx3.2建立了相互抑制的细胞命运,分别促进皮肌节/肌节或骨节的分化。