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EphA 受体信号转导在视皮层拓扑映射过程中的遗传解析。

Genetic dissection of EphA receptor signaling dynamics during retinotopic mapping.

机构信息

Molecular Neurobiology Laboratory, The Salk Institute, La Jolla, California 92037, USA.

出版信息

J Neurosci. 2011 Jul 13;31(28):10302-10. doi: 10.1523/JNEUROSCI.1652-11.2011.

DOI:10.1523/JNEUROSCI.1652-11.2011
PMID:21753007
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3144163/
Abstract

Retinal ganglion cells (RGCs) project axons from their cell bodies in the eye to targets in the superior colliculus of the midbrain. The wiring of these axons to their synaptic targets creates an ordered representation, or "map," of retinal space within the brain. Many lines of experiments have demonstrated that the development of this map requires complementary gradients of EphA receptor tyrosine kinases and their ephrin-A ligands, yet basic features of EphA signaling during mapping remain to be resolved. These include the individual roles played by the multiple EphA receptors that make up the retinal EphA gradient. We have developed a set of ratiometric "relative signaling" (RS) rules that quantitatively predict how the composite low-nasal-to-high-temporal EphA gradient is translated into topographic order among RGCs. A key feature of these rules is that the component receptors of the gradient--in the mouse, EphA4, EphA5, and EphA6--must be functionally equivalent and interchangeable. To test this aspect of the model, we generated compound mutant mice in which the periodicity, slope, and receptor composition of the gradient are systematically altered with respect to the levels of EphA4, EphA5, and a closely related receptor, EphA3, that we ectopically express. Analysis of the retinotopic maps of these new mouse mutants establishes the general utility of the RS rules for predicting retinocollicular topography, and demonstrates that individual EphA gene products are approximately equivalent with respect to axon guidance and target selection.

摘要

视网膜神经节细胞 (RGCs) 将轴突从其眼内的细胞体投射到中脑上丘的靶标。这些轴突与突触靶标的连接形成了大脑内视网膜空间的有序表示或“图谱”。许多实验表明,这种图谱的发育需要 EphA 受体酪氨酸激酶及其 ephrin-A 配体的互补梯度,但 EphA 信号在映射过程中的基本特征仍有待解决。这些特征包括构成视网膜 EphA 梯度的多个 EphA 受体所起的个体作用。我们开发了一套比率“相对信号”(RS)规则,可定量预测复合低鼻侧至高颞侧 EphA 梯度如何转化为 RGC 之间的地形顺序。这些规则的一个关键特征是,梯度的组成受体——在小鼠中为 EphA4、EphA5 和 EphA6——必须具有功能等效性和可互换性。为了测试该模型的这一方面,我们生成了复合突变小鼠,其中梯度的周期性、斜率和受体组成相对于 EphA4、EphA5 和我们异位表达的密切相关受体 EphA3 的水平被系统地改变。这些新的小鼠突变体的视网膜地图分析确立了 RS 规则在预测视网膜-丘脑中的拓扑结构的普遍适用性,并表明单个 EphA 基因产物在轴突导向和靶标选择方面大致相当。

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本文引用的文献

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A simple model can unify a broad range of phenomena in retinotectal map development.一个简单的模型可以统一视网膜顶盖图谱发育中的广泛现象。
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Analysis of mouse EphA knockins and knockouts suggests that retinal axons programme target cells to form ordered retinotopic maps.对小鼠EphA基因敲入和敲除的分析表明,视网膜轴突对靶细胞进行编程,以形成有序的视网膜拓扑图。
Development. 2006 Jul;133(14):2705-17. doi: 10.1242/dev.02430. Epub 2006 Jun 14.
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Evidence for an instructive role of retinal activity in retinotopic map refinement in the superior colliculus of the mouse.视网膜活动在小鼠上丘视网膜拓扑图精细化中起指导性作用的证据。
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