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首页> 外文期刊>Genesis: the journal of genetics and development >miR-199 plays both positive and negative regulatory roles in Xenopus eye development
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miR-199 plays both positive and negative regulatory roles in Xenopus eye development

机译:MiR-199在Xenopus眼部发育中发挥积极和负面的监管作用

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摘要

To investigate microRNA (miR) functions in early eye development, we asked whether eye field transcription factors (EFTFs) are targets of miR-dependent regulation in Xenopus embryos. Argonaute (AGO) ribonucleoprotein complexes, including miRs and targeted mRNAs, were coimmunoprecipitated from transgenic embryos expressing myc-tagged AGO under the control of the rax1 promoter; mRNAs for all EFTFs coimmunoprecipitated with Ago in late neurulae. Computational predictions of miR binding sites within EFTF 3 ' UTRs identified miR-199a-3p ("miR-199") as a candidate regulator of EFTFs, and miR-199 was shown to regulate rax1 in vivo. Targeted overexpression of miR-199 led to small eyes, a reduction in EFTF expression, and reduced cell proliferation. Inhibition of interactions between mir-199 and the rax1 3 ' UTR reversed the small eye phenotype. Although targeted knockdown of miR-199 left the eye field intact, it reduced optic cup outgrowth and disrupted eye formation. Computational identification of candidate miR-199 targets within the Xenopus transcriptome led to the identification of ptk7 as a candidate regulator. Targeted overexpression of ptk7 resulted in abnormal optic cup formation and a reduction or loss of eye development, recapitulating the range of eye phenotypes seen following miR-199 knockdown. Our results indicate that miR-199 plays both positive and negative regulatory roles in eye development.
机译:为了在早期眼新发育中调查MicroRNA(miR)功能,我们询问了眼现场转录因子(EFTFS)是否是异常胚胎胚胎中miR依赖性调节的目标。野核核糖蛋白复合物,包括mir和靶向mRNA,在Rax1启动子的控制下,在表达Myc标记的Myc标记前的转基因胚胎中凝结; MRNA为所有EFTFS在晚期的前期co中抚练。 EFTF 3'UTRS中的MiR结合位点的计算预测鉴定了MiR-199A-3P(“MIR-199”)作为EFFFS的候选调节剂,并且显示MIR-199在体内调节RAX1。 MIR-199的针对性过度表达导致小眼睛,降低EFF表达,降低细胞增殖。抑制miR-199和rax1 3'UTR之间的相互作用逆转小眼表型。虽然MiR-199的有针对性的敲击留下了眼睛场,但它减少了光学杯过度和中断的眼睛形成。宫内节病变体内候选MIR-199靶标的计算鉴定导致PTK7作为候选调节剂的鉴定。 PTK7的靶向过度表达导致视神经杯形成异常和眼部发育的减少或丧失,重新承诺在MiR-199敲低后看到的眼表型范围。我们的结果表明,MIR-199在眼睛发育中起着积极和负面的监管作用。

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