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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Dynamic expression of axon guidance cues required for optic tract development is controlled by fibroblast growth factor signaling.
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Dynamic expression of axon guidance cues required for optic tract development is controlled by fibroblast growth factor signaling.

机译:视神经系统发育所需的轴突指导信号的动态表达是由成纤维细胞生长因子信号控制的。

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摘要

Axons are guided to their targets by molecular cues expressed in their environment. How is the presence of these cues regulated? Although some evidence indicates that morphogens establish guidance cue expression as part of their role in patterning tissues, an important question is whether morphogens are then required to maintain guidance signals. We found that fibroblast growth factor (FGF) signaling sustains the expression of two guidance cues, semaphorin3A (xsema3A) and slit1 (xslit1), throughout the period of Xenopus optic tract development. With FGF receptor inhibition, xsema3A and xslit1 levels were rapidly diminished, and retinal ganglion cell axons arrested in the mid-diencephalon, before reaching their target. Importantly, direct downregulation of XSema3A and XSlit1 mostly phenocopied this axon guidance defect. Thus, FGFs promote continued presence of specific guidance cues critical for normal optic tract development, suggesting a second later role for morphogens, independent of tissue patterning, in maintaining select cues by acting to regulate their transcription.
机译:轴突通过在其环境中表达的分子线索被引导至目标。如何对这些提示的存在进行调节?尽管一些证据表明形态发生子建立指导提示表达,作为其在组织组织模式中的作用的一部分,但一个重要的问题是,是否需要形态发生子来维持指导信号。我们发现,成纤维细胞生长因子(FGF)信号在非洲爪蟾视线发育的整个过程中都维持了两个指导信号semaphorin3A(xsema3A)和split1(xslit1)的表达。通过FGF受体抑制,xsema3A和xslit1水平迅速降低,并且在达到目标之前,视网膜神经节细胞轴突停滞在中脑中部。重要的是,XSema3A和XSlit1的直接下调大多表型化了此轴突指导缺陷。因此,FGFs促进了对正常视力道发育至关重要的特定指导线索的持续存在,这提示了形态发生子的第二个后继作用,独立于组织模式,通过调节其转录来维持选择线索。

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