Sprouty1 和 Sprouty2 通过拮抗 FGF 信号来限制耳嵴和后脑 Wnt8a 的大小。
Sprouty1 and Sprouty2 limit both the size of the otic placode and hindbrain Wnt8a by antagonizing FGF signaling.
机构信息
Department of Pediatrics, Children's Research Institute, Medical College of Wisconsin, 8701 Watertown Plank Road, Milwaukee, WI 53226, USA.
出版信息
Dev Biol. 2011 May 1;353(1):94-104. doi: 10.1016/j.ydbio.2011.02.022. Epub 2011 Feb 26.
Abstract
Multiple signaling molecules, including Fibroblast Growth Factor (FGF) and Wnt, induce two patches of ectoderm on either side of the hindbrain to form the progenitor cell population for the inner ear, or otic placode. Here we report that in Spry1, Spry2 compound mutant embryos (Spry1⁻/⁻; Spry2⁻/⁻ embryos), the otic placode is increased in size. We demonstrate that the otic placode is larger due to the recruitment of cells, normally destined to become cranial epidermis, into the otic domain. The enlargement of the otic placode observed in Spry1⁻/⁻; Spry2⁻/⁻ embryos is preceded by an expansion of a Wnt8a expression domain in the adjacent hindbrain. We demonstrate that both the enlargement of the otic placode and the expansion of the Wnt8a expression domain can be rescued in Spry1⁻/⁻; Spry2⁻/⁻ embryos by reducing the gene dosage of Fgf10. Our results define a FGF-responsive window during which cells can be continually recruited into the otic domain and uncover SPRY regulation of the size of a putative Wnt inductive center.
摘要
多种信号分子,包括成纤维细胞生长因子(FGF)和 Wnt,诱导后脑两侧的两个外胚层区域形成内耳或听基板的祖细胞群体。在这里,我们报告在 Spry1、Spry2 复合突变胚胎(Spry1-/-; Spry2-/- 胚胎)中,听基板的大小增加。我们证明,由于通常注定成为颅表皮的细胞被募集到听基板中,听基板的大小增大。在 Spry1-/-; Spry2-/- 胚胎中观察到的听基板增大之前,相邻后脑中 Wnt8a 表达域的扩张。我们证明,通过降低 Fgf10 的基因剂量,可以在 Spry1-/-; Spry2-/- 胚胎中挽救听基板的增大和 Wnt8a 表达域的扩张。我们的结果定义了一个 FGF 反应性窗口,在此期间可以不断将细胞募集到听基板中,并揭示 SPRY 对假定的 Wnt 诱导中心大小的调节。
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