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通过相反方向的形态发生素梯度实现胚胎模式缩放。

Embryonic pattern scaling achieved by oppositely directed morphogen gradients.

作者信息

McHale Peter, Rappel Wouter-Jan, Levine Herbert

机构信息

Department of Physics and Center for Theoretical Biological Physics, University of California, San Diego, La Jolla, CA 92093-0374, USA.

出版信息

Phys Biol. 2006 May 16;3(2):107-20. doi: 10.1088/1478-3975/3/2/003.

Abstract

Morphogens are proteins, often produced in a localized region, whose concentrations spatially demarcate regions of differing gene expression in developing embryos. The boundaries of gene expression are typically sharp and the genes can be viewed as abruptly switching from on to off or vice versa upon crossing the boundary. To ensure the viability of the organism these boundaries must be set at certain fractional positions within the corresponding developing field. Remarkably this can be done with high precision despite the fact that the size of the developing field itself can vary widely from embryo to embryo. How this scaling is accomplished is unknown but it is clear that a single morphogen gradient is insufficient. Here we show how a pair of morphogens A and B, produced at opposite ends of a one-dimensional developing field, can solve the pattern-scaling problem. In the most promising scenario the morphogens interact via an effective annihilation reaction A + B --> slashed circle and the switch occurs according to the absolute concentration of A or B. We define a scaling criterion and show that morphogens coupled in this way can set embryonic markers across the entire developing field in proportion to the field size. This scaling occurs at developing-field sizes of a few times the morphogen decay length. The scaling criterion is not met if instead the gradients couple combinatorially such that downstream genes are regulated by the ratio A/B of the morphogen concentrations.

摘要

形态发生素是一类蛋白质,通常在局部区域产生,其浓度在空间上划分出发育胚胎中不同基因表达的区域。基因表达的边界通常很清晰,并且这些基因可以被视为在跨越边界时突然从开启状态转变为关闭状态,反之亦然。为确保生物体的生存能力,这些边界必须设置在相应发育区域内的特定分数位置。值得注意的是,尽管发育区域的大小在不同胚胎之间可能有很大差异,但这一过程仍能高精度地完成。目前尚不清楚这种尺度缩放是如何实现的,但很明显单一的形态发生素梯度是不够的。在这里,我们展示了一对在一维发育区域两端产生的形态发生素A和B如何解决模式缩放问题。在最有前景的情况下,形态发生素通过有效的湮灭反应A + B → 空集相互作用,并且开关根据A或B的绝对浓度发生。我们定义了一个缩放标准,并表明以这种方式耦合的形态发生素可以根据区域大小按比例在整个发育区域设置胚胎标记。这种缩放发生在形态发生素衰减长度的几倍的发育区域大小。如果梯度以组合方式耦合,使得下游基因由形态发生素浓度的比值A/B调节,则不满足缩放标准。

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