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Wnt signals mediate a fate decision between otic placode and epidermis.

机译:Wnt信号介导耳底和表皮之间的命运决定。

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The otic placode, the anlagen of the inner ear, develops from an ectodermal field characterized by expression of the transcription factor Pax2. Previous fate mapping studies suggest that these Pax2(+) cells will give rise to both otic placode tissue and epidermis, but the signals that divide the Pax2(+) field into placodal and epidermal territories are unknown. We report that Wnt signaling is normally activated in a subset of Pax2(+) cells, and that conditional inactivation of beta-catenin in these cells causes an expansion of epidermal markers at the expense of the otic placode. Conversely, conditional activation of beta-catenin in Pax2(+) cells causes an expansion of the otic placode at the expense of epidermis, and the resulting otic tissue expresses exclusively dorsal otocyst markers. Together, these results suggest that Wnt signaling acts instructively to direct Pax2(+) cells to an otic placodal, rather than an epidermal, fate and promotes dorsal cell identities in the otocyst.
机译:耳内斑,内耳的胶原蛋白,是从一个以表达转录因子Pax2为特征的外胚层区域发育而来的。先前的命运图谱研究表明,这些Pax2(+)细胞会同时引起耳底斑块组织和表皮,但是将Pax2(+)场分为斑状和表皮区域的信号尚不清楚。我们报告说,Wnt信号通常在Pax2(+)细胞的一个子集中被激活,并且这些细胞中的β-catenin的条件失活会导致表皮标记物的扩展,但会损害耳廓。相反,在Pax2(+)细胞中有条件激活β-catenin会导致以表皮为代价扩大耳道斑的扩展,并且导致的耳道组织仅表达背侧耳囊标志物。在一起,这些结果表明Wnt信号具有指导意义,可将Pax2(+)细胞定向到耳pl,而不是表皮命运,并促进耳囊中的背细胞身份。

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