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Probabilistic splicing of Dscam1 establishes identity at the level of single neurons

机译:Dscam1的概率剪接在单个神经元的水平上建立身份

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摘要

The Drosophila Dscam1 gene encodes a vast number of cell recognition molecules through alternative splicing. These exhibit isoform-specific homophilic binding and regulate self-avoidance, the tendency of neurites from the same cell to repel one another. Genetic experiments indicate that different cells must express different isoforms. How this is achieved is unknown, as expression of alternative exons in vivo has not been shown. Here, we modified the endogenous Dscam1 locus to generate splicing reporters for all variants of exon 4. We demonstrate that splicing does not occur in a cell-type-specific fashion, that cells sharing the same anatomical location in different individuals express different exon 4 variants, and that the splicing pattern in a given neuron can change over time. We conclude that splicing is probabilistic. This is compatible with a widespread role in neural circuit assembly through self-avoidance and is incompatible with models in which specific isoforms of Dscam1 mediate homophilic recognition between processes of different cells.
机译:果蝇Dscam1基因通过选择性剪接编码大量细胞识别分子。它们表现出同种型特异性的同源结合并调节自我回避,即来自同一细胞的神经突相互排斥的趋势。遗传实验表明,不同的细胞必须表达不同的同工型。由于尚未显示体内替代外显子的表达,因此如何实现这一点尚不清楚。在这里,我们修改了内源性Dscam1基因座,以生成外显子4所有变体的剪接报告基因。我们证明了剪接并不是以细胞类型特异性的方式发生的,在不同个体中共享相同解剖位置的细胞表达了不同的外显子4变体。 ,并且给定神经元中的剪接模式可以随时间变化。我们得出结论,剪接是概率性的。这与通过自我回避在神经回路组装中的广泛作用兼容,并且与其中Dscam1的特定同工型介导不同细胞之间的同源识别的模型不兼容。

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