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首页> 外文期刊>Developmental cell >The frizzled extracellular domain is a ligand for Van Gogh/Stbm during nonautonomous planar cell polarity signaling.
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The frizzled extracellular domain is a ligand for Van Gogh/Stbm during nonautonomous planar cell polarity signaling.

机译:卷曲的细胞外结构域是非自主平面细胞极性信号传导过程中梵高/ Stbm的配体。

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摘要

The Frizzled (Fz) receptor is required cell autonomously in Wnt/beta-catenin and planar cell polarity (PCP) signaling. In addition to these requirements, Fz acts nonautonomously during PCP establishment: wild-type cells surrounding fz(-) patches reorient toward the fz(-) cells. The molecular mechanism(s) of nonautonomous Fz signaling are unknown. Our in vivo studies identify the extracellular domain (ECD) of Fz, in particular its CRD (cysteine rich domain), as critical for nonautonomous Fz-PCP activity. Importantly, we demonstrate biochemical and physical interactions between the FzECD and the transmembrane protein Van Gogh/Strabismus (Vang/Stbm). We show that this function precedes cell-autonomous interactions and visible asymmetric PCP factor localization. Our data suggest that Vang/Stbm can act as a FzECD receptor, allowing cells to sense Fz activity/levels of their neighbors. Thus, direct Fz-Vang/Stbm interactions represent an intriguing mechanism that may account for the global orientation of cells within the plane of their epithelial field.
机译:卷曲(Fz)受体是Wnt /β-catenin和平面细胞极性(PCP)信号传导中自主需要的细胞。除了这些要求之外,Fz在PCP建立过程中也不会自动起作用:围绕fz(-)补丁的野生型细胞会重新定向到fz(-)细胞。非自治Fz信号传导的分子机制是未知的。我们的体内研究确定Fz的胞外域(ECD),尤其是其CRD(富含半胱氨酸的域),对于非自主Fz-PCP活性至关重要。重要的是,我们证明了FzECD与跨膜蛋白Van Gogh / Strabismus(Vang / Stbm)之间的生化和物理相互作用。我们显示此功能先于细胞自主相互作用和可见的不对称PCP因子定位。我们的数据表明,Vang / Stbm可以充当FzECD受体,使细胞能够感知其邻居的Fz活性/水平。因此,直接的Fz-Vang / Stbm相互作用代表了一种有趣的机制,可以解释细胞在其上皮视野内的整体方向。

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