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sfrp1 通过负反馈调控 Wnt 信号促进非洲爪蟾心肌细胞分化。

sfrp1 promotes cardiomyocyte differentiation in Xenopus via negative-feedback regulation of Wnt signalling.

机构信息

Institute of Medical Sciences, University of Aberdeen, Aberdeen AB25 2ZD, UK.

出版信息

Development. 2013 Apr;140(7):1537-49. doi: 10.1242/dev.088047.

Abstract

Wnt signalling is a key regulator of vertebrate heart development, yet it is unclear which specific Wnt signalling components are required to regulate which aspect of cardiogenesis. Previously, we identified Wnt6 as an endogenous Wnt ligand required for controlling heart muscle differentiation via canonical Wnt/β-catenin signalling. Here we show for the first time a requirement for an endogenous Wnt signalling inhibitor for normal heart muscle differentiation. Expression of sfrp1 is strongly induced in differentiating heart muscle. We show that sfrp1 is not only able to promote heart muscle differentiation but is also required for the formation of normal size heart muscle in the embryo. sfrp1 is functionally able to inhibit Wnt6 signalling and its requirement during heart development relates to relieving the cardiogenesis-restricting function of endogenous wnt6. In turn, we discover that sfrp1 expression in the heart is regulated by Wnt6 signalling, which for the first time indicates that sfrp genes can function as part of a Wnt negative-feedback regulatory loop. Our experiments indicate that sfrp1 controls the size of the differentiating heart muscle primarily by regulating cell fate within the cardiac mesoderm between muscular and non-muscular cell lineages. The cardiac mesoderm is therefore not passively patterned by signals from the surrounding tissue, but regulates its differentiation into muscular and non-muscular tissue using positional information from the surrounding tissue. This regulatory network might ensure that Wnt activation enables expansion and migration of cardiac progenitors, followed by Wnt inhibition permitting cardiomyocyte differentiation.

摘要

Wnt 信号通路是脊椎动物心脏发育的关键调节剂,但尚不清楚哪些特定的 Wnt 信号通路成分需要调节心脏发生的哪个方面。以前,我们鉴定出 Wnt6 作为一种内源性 Wnt 配体,通过经典的 Wnt/β-catenin 信号通路来控制心肌分化。在这里,我们首次证明了内源性 Wnt 信号通路抑制剂对于正常心肌分化是必需的。Sfrp1 的表达在分化的心肌中强烈诱导。我们表明,Sfrp1 不仅能够促进心肌分化,而且对于胚胎中正常大小的心肌形成也是必需的。Sfrp1 在功能上能够抑制 Wnt6 信号通路,其在心脏发育过程中的需求与缓解内源性 wnt6 的心脏发生限制功能有关。反过来,我们发现 Sfrp1 在心脏中的表达受 Wnt6 信号通路的调节,这首次表明 Sfrp 基因可以作为 Wnt 负反馈调节环的一部分发挥作用。我们的实验表明,Sfrp1 主要通过调节心脏中中胚层的细胞命运来控制正在分化的心肌的大小,在心肌中,细胞命运在肌肉和非肌肉细胞谱系之间进行调节。因此,心脏中胚层不是被动地受到周围组织信号的影响,而是利用周围组织的位置信息来调节其分化为肌肉和非肌肉组织。这个调节网络可能确保 Wnt 激活能够使心脏祖细胞扩张和迁移,随后 Wnt 抑制允许心肌细胞分化。

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