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Parallel imaging of Drosophila embryos for quantitative analysis of genetic perturbations of the Ras pathway

机译:果蝇胚胎的并行成像,用于定量分析Ras途径的遗传扰动

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The Ras pathway patterns the poles of the Drosophila embryo by downregulating the levels and activity of a DNA-binding transcriptional repressor Capicua (Cic). We demonstrate that the spatiotemporal pattern of Cic during this signaling event can be harnessed for functional studies of mutations in the Ras pathway in human diseases. Our approach relies on a new microfluidic device that enables parallel imaging of Cic dynamics in dozens of live embryos. We found that although the pattern of Cic in early embryos is complex, it can be accurately approximated by a product of one spatial profile and one time-dependent amplitude. Analysis of these functions of space and time alone reveals the differential effects of mutations within the Ras pathway. Given the highly conserved nature of Ras-dependent control of Cic, our approach provides new opportunities for functional analysis of multiple sequence variants from developmental abnormalities and cancers.
机译:Ras途径通过下调结合DNA的转录阻遏物Capicua(Cic)的水平和活性,在果蝇胚胎的两极上形成图案。我们证明在此信号事件期间Cic的时空模式可以用于人类疾病中Ras途径突变的功能研究。我们的方法依赖于一种新的微流体设备,该设备能够对数十个活胚胎中的Cic动态进行并行成像。我们发现,尽管早期胚胎中Cic的模式很复杂,但可以通过一个空间轮廓和一个随时间变化的幅度的乘积来精确地近似。仅对时空的这些功能进行的分析揭示了Ras途径内突变的不同影响。鉴于Ras依赖Cic的控制的高度保守的性质,我们的方法为来自发育异常和癌症的多个序列变异的功能分析提供了新的机会。

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