建立 Bicoid 梯度模型。
Modelling the Bicoid gradient.
机构信息
Howard Hughes Medical Institute, Department of Molecular Biology, Princeton University, Princeton, NJ 08544, USA.
出版信息
Development. 2010 Jul;137(14):2253-64. doi: 10.1242/dev.032409.
Abstract
Morphogen gradients provide embryonic tissues with positional information by inducing target genes at different concentration thresholds and thus at different positions. The Bicoid morphogen gradient in Drosophila melanogaster embryos has recently been analysed quantitatively, yet how it forms remains a matter of controversy. Several biophysical models that rely on production, diffusion and degradation have been formulated to account for the observed dynamics of the Bicoid gradient, but no one model can account for all its characteristics. Here, we discuss how existing data on this gradient fit the various proposed models and what aspects of gradient formation these models fail to explain. We suggest that knowing a few additional parameters, such as the lifetime of Bicoid, would help to identify and develop better models of Bicoid gradient formation.
摘要
形态发生素梯度通过在不同浓度阈值下诱导靶基因,从而在不同位置为胚胎组织提供位置信息。最近对黑腹果蝇胚胎中的 Bicoid 形态发生素梯度进行了定量分析,但它是如何形成的仍然存在争议。已经提出了几种依赖于产生、扩散和降解的生物物理模型来解释 Bicoid 梯度的观察到的动力学,但没有一个模型可以解释其所有特征。在这里,我们讨论了这些梯度的现有数据如何适应各种提出的模型,以及这些模型未能解释梯度形成的哪些方面。我们建议,了解一些额外的参数,如 Bicoid 的寿命,将有助于确定和开发更好的 Bicoid 梯度形成模型。
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