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首页> 外文期刊>Development >Hox control of morphogen mobility and organ development through regulation of glypican expression.
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Hox control of morphogen mobility and organ development through regulation of glypican expression.

机译:Hox通过调节Glypican表达来控制形态发生子的活动性和器官发育。

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Animal bodies are composed of structures that vary in size and shape within and between species. Selector genes generate these differences by altering the expression of effector genes whose identities are largely unknown. Prime candidates for such effector genes are components of morphogen signaling pathways, which control growth and patterning during development. Here we show that in Drosophila the Hox selector gene Ultrabithorax (Ubx) modulates morphogen signaling in the haltere through transcriptional regulation of the glypican dally. Ubx, in combination with the posterior selector gene engrailed (en), represses dally expression in the posterior (P) compartment of the haltere. Compared with the serially homologous wing, where Ubx is not expressed, low levels of posterior dally in the haltere contribute to a reduced P compartment size and an overall smaller appendage size. We also show that one molecular consequence of dally repression in the posterior haltere is to reduce Dpp diffusion into and through the P compartment. Our results suggest that Dpp mobility is biased towards cells with higher levels of Dally and that selector genes modulate organ development by regulating glypican levels.
机译:动物的身体由物种内部和物种之间大小和形状变化的结构组成。选择基因通过改变效应基因的表达而产生这些差异,这些效应基因的身份很大程度上未知。此类效应基因的主要候选物是吗啡信号转导途径的组成部分,其在发育过程中控制生长和模式。在这里,我们显示在果蝇中,Hox选择基因Ultrabithorax(Ubx)通过glypican dally的转录调控来调节中的形态发生信号。 Ubx与引入的后选择基因(en)结合,可抑制三角ter后(P)区室中的Dally表达。与未表达Ubx的系列同源翼相比,吊带衫中较低的后导板水平有助于减小P隔室的尺寸,并总体上减小附件的尺寸。我们还表明,在后部进行双板压制的一种分子结果是减少了Dpp扩散进和通过P隔室。我们的结果表明,Dpp流动性偏向于具有较高Dally水平的细胞,并且选择基因通过调节Glypican水平来调节器官发育。

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