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通过酶-底物相互作用塑造 BMP 形态发生梯度。

Shaping BMP morphogen gradients through enzyme-substrate interactions.

机构信息

Program in Cellular Regulation and Metabolism, NICHD, NIH, Bethesda, MD 20892, USA.

出版信息

Dev Cell. 2011 Aug 16;21(2):375-83. doi: 10.1016/j.devcel.2011.06.025.

Abstract

Bone morphogenetic proteins (BMPs) regulate dorsal/ventral (D/V) patterning across the animal kingdom; however, the biochemical properties of certain pathway components can vary according to species-specific developmental requirements. For example, Tolloid (Tld)-like metalloproteases cleave vertebrate BMP-binding proteins called Chordins constitutively, while the Drosophila Chordin ortholog, Short gastrulation (Sog), is only cleaved efficiently when bound to BMPs. We identified Sog characteristics responsible for making its cleavage dependent on BMP binding. "Chordin-like" variants that are processed independently of BMPs changed the steep BMP gradient found in Drosophila embryos to a shallower profile, analogous to that observed in some vertebrate embryos. This change ultimately affected cell fate allocation and tissue size and resulted in increased variability of patterning. Thus, the acquisition of BMP-dependent Sog processing during evolution appears to facilitate long-range ligand diffusion and formation of a robust morphogen gradient, enabling the bistable BMP signaling outputs required for early Drosophila patterning.

摘要

骨形态发生蛋白(BMPs)在整个动物界中调节背/腹(D/V)模式;然而,某些途径成分的生化特性可能根据物种特异性的发育要求而有所不同。例如,Tolloid(Tld)样金属蛋白酶持续切割脊椎动物 BMP 结合蛋白称为 Chordin,而果蝇 Chordin 同源物 Short gastrulation(Sog)只有在与 BMP 结合时才能有效地被切割。我们确定了 Sog 的特征,这些特征使其切割依赖于 BMP 结合。“Chordin 样”变体独立于 BMP 进行加工,将在果蝇胚胎中发现的陡峭 BMP 梯度改变为更浅的轮廓,类似于在一些脊椎动物胚胎中观察到的情况。这种变化最终影响了细胞命运分配和组织大小,并导致了模式形成的更大可变性。因此,在进化过程中获得 BMP 依赖性 Sog 加工似乎促进了长距离配体扩散和形成强大的形态发生梯度,从而为早期果蝇模式形成提供了所需的双稳态 BMP 信号输出。

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