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测量和扰动形态发生素寿命:对梯度形状的影响。

Measurement and perturbation of morphogen lifetime: effects on gradient shape.

机构信息

Lewis-Sigler Institute for Integrative Genomics, Princeton University, Princeton, New Jersey, USA.

出版信息

Biophys J. 2011 Oct 19;101(8):1807-15. doi: 10.1016/j.bpj.2011.07.025.

DOI:10.1016/j.bpj.2011.07.025
PMID:22004733
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3192964/
Abstract

Protein lifetime is of critical importance for most biological processes and plays a central role in cell signaling and embryonic development, where it impacts the absolute concentration of signaling molecules and, potentially, the shape of morphogen gradients. Early conceptual and mathematical models of gradient formation proposed that steady-state gradients are established by an equilibration between the lifetime of a morphogen and its rates of synthesis and diffusion, though whether gradients in fact reach steady state before being read out is a matter of controversy. In any case, this class of models predicts that protein lifetime is a key determinant of both the time to steady state and the spatial extent of a gradient. Using a method that employs repeated photoswitching of a fusion of the morphogen Bicoid (Bcd) and the photoconvertible fluorescent protein Dronpa, we measure and modify the lifetime of Dronpa-Bcd in living Drosophila embryos. We find that the lifetime of Bcd is dynamic, changing from 50 min before mitotic cycle 14 to 15 min during cellularization. Moreover, by measuring total quantities of Bcd over time, we find that the gradient does not reach steady state. Finally, using a nearly continuous low-level conversion to the dark state of Dronpa-Bcd to mimic the effect of increased degradation, we demonstrate that perturbation of protein lifetime changes the characteristic length of the gradient, providing direct support for a mechanism based on synthesis, diffusion, and degradation.

摘要

蛋白质寿命对大多数生物过程至关重要,在细胞信号转导和胚胎发育中发挥核心作用,影响信号分子的绝对浓度,并可能影响形态发生梯度的形状。早期关于梯度形成的概念和数学模型提出,通过形态发生物的寿命与其合成和扩散速率之间的平衡来建立稳定状态的梯度,尽管在被读出之前梯度实际上是否达到稳定状态是一个有争议的问题。在任何情况下,这类模型都预测蛋白质寿命是达到稳定状态的时间和梯度空间范围的关键决定因素。我们使用一种方法,该方法采用融合形态发生物 Bicoid(Bcd)和光可转化荧光蛋白 Dronpa 的重复光开关,测量并修改活果蝇胚胎中 Dronpa-Bcd 的寿命。我们发现 Bcd 的寿命是动态的,从有丝分裂周期 14 之前的 50 分钟变化到细胞化期间的 15 分钟。此外,通过随时间测量 Bcd 的总量,我们发现梯度未达到稳定状态。最后,通过对 Dronpa-Bcd 进行近乎连续的低水平转换为暗态来模拟降解增加的影响,我们证明了蛋白质寿命的扰动会改变梯度的特征长度,为基于合成、扩散和降解的机制提供了直接支持。

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本文引用的文献

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The formation of the Bicoid morphogen gradient requires protein movement from anteriorly localized mRNA.Bicoid 形态发生素梯度的形成需要蛋白质从前部定位的 mRNA 中移动。
PLoS Biol. 2011 Mar;9(3):e1000596. doi: 10.1371/journal.pbio.1000596. Epub 2011 Mar 1.
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How long does it take to establish a morphogen gradient?建立形态发生梯度需要多长时间?
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High mobility of bicoid captured by fluorescence correlation spectroscopy: implication for the rapid establishment of its gradient.荧光相关光谱技术捕获的高迁移率的bicoid:对其快速建立梯度的启示。
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