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首页> 外文期刊>BMC Developmental Biology >Pax4 is not essential for beta-cell differentiation in zebrafish embryos but modulates alpha-cell generation by repressing arx gene expression
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Pax4 is not essential for beta-cell differentiation in zebrafish embryos but modulates alpha-cell generation by repressing arx gene expression

机译:Pax4对于斑马鱼胚胎中的β细胞分化不是必需的,但可以通过抑制arx基因表达来调节α细胞的生成

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Background Genetic studies in mouse have demonstrated the crucial function of PAX4 in pancreatic cell differentiation. This transcription factor specifies β- and δ-cell fate at the expense of α-cell identity by repressing Arx gene expression and ectopic expression of PAX4 in α-cells is sufficient to convert them into β-cells. Surprisingly, no Pax4 orthologous gene can be found in chicken and Xenopus tropicalis raising the question of the function of pax4 gene in lower vertebrates such as in fish. In the present study, we have analyzed the expression and the function of the orthologous pax4 gene in zebrafish. Results pax4 gene is transiently expressed in the pancreas of zebrafish embryos and is mostly restricted to endocrine precursors as well as to some differentiating δ- and ε-cells but was not detected in differentiating β-cells. pax4 knock-down in zebrafish embryos caused a significant increase in α-cells number while having no apparent effect on β- and δ-cell differentiation. This rise of α-cells is due to an up-regulation of the Arx transcription factor. Conversely, knock-down of arx caused to a complete loss of α-cells and a concomitant increase of pax4 expression but had no effect on the number of β- and δ-cells. In addition to the mutual repression between Arx and Pax4, these two transcription factors negatively regulate the transcription of their own gene. Interestingly, disruption of pax4 RNA splicing or of arx RNA splicing by morpholinos targeting exon-intron junction sites caused a blockage of the altered transcripts in cell nuclei allowing an easy characterization of the arx- and pax4-deficient cells. Such analyses demonstrated that arx knock-down in zebrafish does not lead to a switch of cell fate, as reported in mouse, but rather blocks the cells in their differentiation process towards α-cells. Conclusions In zebrafish, pax4 is not required for the generation of the first β- and δ-cells deriving from the dorsal pancreatic bud, unlike its crucial role in the differentiation of these cell types in mouse. On the other hand, the mutual repression between Arx and Pax4 is observed in both mouse and zebrafish. These data suggests that the main original function of Pax4 during vertebrate evolution was to modulate the number of pancreatic α-cells and its role in β-cells differentiation appeared later in vertebrate evolution.
机译:背景技术小鼠遗传学研究证明PAX4在胰腺细胞分化中起着至关重要的作用。该转录因子通过抑制Arx基因表达而以α细胞同一性为代价指定了β细胞和δ细胞的命运,PAX4在α细胞中的异位表达足以将它们转化为β细胞。出人意料的是,在鸡和热带非洲爪蟾中没有发现Pax4直系同源基因,这提出了在低等脊椎动物如鱼类中pax4基因功能的问题。在本研究中,我们分析了直系同源pax4基因在斑马鱼中的表达和功能。结果pax4基因在斑马鱼胚胎的胰腺中瞬时表达,并且主要限于内分泌前体以及某些分化的δ和ε细胞,但在分化的β细胞中未检测到。斑马鱼胚胎中的pax4敲低导致α细胞数量的显着增加,而对β细胞和δ细胞的分化没有明显影响。 α细胞的这种上升是由于Arx转录因子的上调所致。相反,敲除arx会导致α细胞完全丢失,并伴随pax4表达增加,但对β细胞和δ细胞的数量没有影响。除了Arx和Pax4之间的相互抑制外,这两个转录因子还负面调节其自身基因的转录。有趣的是,通过靶向外显子-内含子连接位点的吗啉代对pax4 RNA剪接或arx RNA剪接的破坏导致细胞核中改变的转录物被阻滞,从而易于表征arx和pax4缺陷细胞。此类分析表明,斑马鱼中的arx基因敲除不会导致细胞命运的改变(如小鼠中报道的那样),而是会阻止细胞向α细胞的分化过程。结论在斑马鱼中,pax4不是从胰背芽衍生的第一个β细胞和δ细胞的生成所必需的,这与其在小鼠中区分这些细胞类型的关键作用不同。另一方面,在小鼠和斑马鱼中都观察到Arx​​和Pax4之间的相互抑制。这些数据表明,Pax4在脊椎动物进化过程中的主要原始功能是调节胰腺α细胞的数量,并且其在β细胞分化中的作用出现在脊椎动物进化的后期。

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