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Gastrulation in rabbit blastocysts depends on insulin and insulin-like-growth-factor 1

机译:兔胚泡的排卵取决于胰岛素和胰岛素样生长因子1

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Insulin and insulin-like-growth-factor 1 (IGF1) are components of the uterine secretions. As potent growth factors they influence early embryo development. The underlying molecular mechanisms are largely unknown. Here we report on the effects of insulin and IGF1 on early gastrulation in rabbit blastocysts. We have studied blastocysts grown in vivo in metabolically healthy rabbits, in rabbits with type 1 diabetes and in vitro in the presence or absence of insulin or IGF1. Embryonic disc morphology and expression of Brachyury, Wnt3a and Wnt4 were analysed by qPCR and IHC.Pre-gastrulated blastocysts (stage 0/1) cultured with insulin or IGF1 showed a significantly higher capacity to form the posterior mesoderm and primitive streak (stage 2 and 3) than blastocysts cultured without growth factors. In gastrulating blastocysts the levels of the mesoderm-specific transcription factor Brachyury and the Wnt signalling molecules Wnt3a and Wnt4 showed a stage-specific expression pattern with Brachyury transcripts increasing from stage 0/1 to 3. Wnt4 protein was found spread over the whole embryoblast. Insulin induced Wnt3a, Wnt4 and Brachyury expression in a temporal- and stage-specific pattern. Only blastocysts cultured with insulin reached the Wnt3a, Wnt4 and Brachyury expression levels of stage 2 in vivo blastocysts, indicating that insulin is required for Wnt3a, Wnt4 and Brachyury expression during gastrulation. Insulin-induced Wnt3a and Wnt4 expression preceded Brachyury. Wnt3a-induced expression could be depleted by MEK1 inhibition (PD98059). Involvement of insulin in embryonic Wnt3a expression was further shown in vivo with Wnt3a expression being notably down regulated in stage 2 blastocysts from rabbits with type 1 diabetes.Blastocysts grown in diabetic rabbits are retarded in development, a finding which supports our current results that insulin is highly likely required for early mesoderm formation in rabbit blastocysts by inducing a distinct spatiotemporal expression profile of Wnt3a, Wnt4 and Brachyury.
机译:胰岛素和胰岛素样生长因子1(IGF1)是子宫分泌物的组成部分。作为有效的生长因子,它们影响早期胚胎的发育。潜在的分子机制很大程度上未知。在这里,我们报道了胰岛素和IGF1对家兔胚泡早期胃形成的影响。我们研究了在代谢健康的兔子,患有1型糖尿病的兔子体内以及在有或没有胰岛素或IGF1的情况下体外生长的胚泡。通过qPCR和IHC分析了胚盘的形态以及Brachyury,Wnt3a和Wnt4的表达。用胰岛素或IGF1培养的预妊娠胚泡(0/1期)显示出明显更高的形成中胚层和原始条带的能力(2期3)比胚泡培养无生长因子。在囊胚性胚泡中,中胚层特异性转录因子Brachyury和Wnt信号分子Wnt3a和Wnt4表现出阶段特异性表达模式,其中Brachyury转录物从0/1阶段增加到3阶段。发现Wnt4蛋白遍布整个胚胚。胰岛素以时间和阶段特异性模式诱导Wnt3a,Wnt4和Brachyury表达。只有用胰岛素培养的胚泡才能达到体内胚泡第2阶段的Wnt3a,Wnt4和Brachyury表达水平,这表明在胃泌乳过程中Wnt3a,Wnt4和Brachyury表达需要胰岛素。胰岛素诱导的Wnt3a和Wnt4表达先于Brachyury。 Wnt3a诱导的表达可能被MEK1抑制(PD98059)耗尽。体内胰岛素进一步参与了胚胎Wnt3a表达的研究,其中Wnt3a表达在1型糖尿病兔的2期胚泡中明显下调。通过诱导Wnt3a,Wnt4和Brachyury的独特的时空表达模式,在兔胚囊的早期中胚层形成中非常需要。

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