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Shaping a Morphogen Gradient for Positional Precision

机译:调整Morphogen梯度以提高位置精度

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摘要

Morphogen gradients, which provide positional information to cells in a developing tissue, could in principle adopt any nonuniform profile. To our knowledge, how the profile of a morphogen gradient affects positional precision has not been well studied experimentally. Here, we compare the positional precision provided by the Drosophila morphogenetic protein Bicoid (Bcd) in wild-type (wt) embryos with embryos lacking an interacting cofactor. The Bcd gradient in the latter case exhibits decreased positional precision around mid-embryo compared with its wt counterpart. The domain boundary of Hunchback (Hb), a target activated by Bcd, becomes more variable in mutant embryos. By considering embryo-to-embryo, internal, and measurement fluctuations, we dissect mathematically the relevant sources of fluctuations that contribute to the error in positional information. Using this approach, we show that the defect in Hb boundary positioning in mutant embryos is directly reflective of an altered Bcd gradient profile with increasing flatness toward mid-embryo. Furthermore, we find that noise in the Bcd input signal is dominated by internal fluctuations but, due to time and spatial averaging, the spatial precision of the Hb boundary is primarily affected by embryo-to-embryo variations. Our results demonstrate that the positional information provided by the wt Bcd gradient profile is highly precise and necessary for patterning precision.
机译:形态梯度可为发育中的组织中的细胞提供位置信息,原则上可以采用任何不均匀的轮廓。据我们所知,尚未对形态发生子梯度的轮廓如何影响位置精度进行深入研究。在这里,我们比较了果蝇形态发生蛋白Bicoid(Bcd)在野生型(wt)胚胎中与缺少相互作用辅因子的胚胎所提供的位置精度。在后者的情况下,Bcd梯度与其wt对应物相比在中胚周围的位置精度降低。驼背(Hb)(由Bcd激活的靶标)的域边界在突变胚胎中变得更加可变。通过考虑胚胎到胚胎的,内部的和测量的波动,我们在数学上剖析了导致位置信息错误的波动的相关来源。使用这种方法,我们表明突变体胚胎中Hb边界定位的缺陷直接反映了Bcd梯度分布的变化,并朝着中胚方向增加了平坦度。此外,我们发现Bcd输入信号中的噪声主要受内部波动的影响,但是由于时间和空间平均,Hb边界的空间精度主要受胚胎间差异的影响。我们的结果表明,wt Bcd梯度轮廓提供的位置信息非常精确,并且对于构图精度是必需的。

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