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WNT8 and BMP2B co-regulate non-axial mesoderm patterning during zebrafish gastrulation.

机译:WNT8和BMP2B共同调节斑马鱼胃成膜过程中的非轴向中胚层模式。

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摘要

During vertebrate mesoderm formation, fates are established according to position in the dorsoventral (D/V) axis of the embryo. Initially, maternal signaling divides nascent mesoderm into axial (dorsal) and non-axial (ventral) domains. Although the subsequent subdivision of non-axial mesoderm into multiple D/V fate domains is known to involve zygotic Wnt8 and BMP signaling as well as the Vent/Vox/Ved family of transcriptional repressors, how levels of signaling activity are translated into differential regulation of fates is not well understood. To address this question, we have analyzed zebrafish embryos lacking Wnt8 and BMP2b. Zebrafish wnt8; swr (bmp2b) double mutants display a progressive loss of non-axial mesoderm and a concomitant expansion of axial mesoderm during gastrulation. Mesoderm induction and specification of the axial domain occur normally in wnt8; swr mutants, but dorsal mesoderm genes eventually come to be expressed throughout the mesoderm, suggesting that the establishment of non-axial mesoderm identity requires continual repression of dorsal mesoderm factors, including repressors of ventral genes. Loss-of-function for Vent, Vox, and Ved phenocopies the wnt8; swr mutant phenotype, consistent with Wnt8 and BMP2b maintaining non-axial mesoderm identity during gastrulation through the regulation of these three transcriptional repressors. We postulate that timely differentiation of the mesoderm requires the maintenance of non-axial mesoderm identity by Wnt8 and BMP2b at the onset of gastrulation followed by subdivision of the non-axial mesoderm into different functional domains during gastrulation.
机译:在脊椎动物中胚层形成过程中,根据胚胎在背腹(D / V)轴上的位置确定命运。最初,母体信号传导将新生的中胚层分为轴向(背侧)和非轴向(腹侧)域。尽管随后将非轴向中胚层细分为多个D / V命运域涉及合子Wnt8和BMP信号转导以及Vent / Vox / Ved家族的转录阻遏物,但信号转导水平如何转化为对Dnt的差异调节。命运还不很清楚。为了解决这个问题,我们分析了缺少Wnt8和BMP2b的斑马鱼胚胎。斑马鱼wnt8; swr(bmp2b)双重突变体在胃胚形成过程中显示出非轴向中胚层的逐渐丧失和轴向中胚层的同时扩张。中胚层感应和轴向域规范通常发生在wnt8中; swr突变体,但背中胚层基因最终在整个中胚层中表达,这表明建立非轴向中胚层身份需要不断抑制背中胚层因子,包括腹侧基因的阻遏物。 Vnt,Vox和Ved表型丧失了wnt8的功能; swr突变体表型,与Wnt8和BMP2b一致,通过调节这三个转录阻遏物,在胃肠形成过程中保持非轴向中胚层身份。我们假设中胚层的及时分化需要在胃芽形成开始时通过Wnt8和BMP2b维持非轴向中胚层的身份,然后在胃芽形成期间将非轴向中胚层细分为不同的功能域。

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