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Two-step selection of a single R8 photoreceptor: a bistable loop between senseless and rough locks in R8 fate

机译:单个R8感光器的两步选择:R8命运中无意义的锁定和粗糙锁定之间的双稳态回路

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摘要

Patterning of sensory organs requires precise regulation of neural induction and repression. The neurocrystalline pattern of the adult Drosophila compound eye is generated by ordered selection of single founder photoreceptors (R8s) for each unit eye or ommatidium. R8 selection requires mechanisms that restrict R8 potential to a single cell from within a group of cells expressing the proneural gene atonal (ato). One model of R8 selection suggests that R8 precursors are selected from a three-cell ‘R8 equivalence group’ through repression of ato by the homeodomain transcription factor Rough (Ro). A second model proposes that lateral inhibition is sufficient to select a single R8 from an equipotent group of cells called the intermediate group (IG). Here, we provide new evidence that lateral inhibition, but not ro, is required for the initial selection of a single R8 precursor. We show that in ro mutants, ectopic R8s develop from R2,5 photoreceptor precursors independently of ectopic Ato and hours after normal R8s are specified. We also show that Ro directly represses the R8 specific zinc-finger transcription factor senseless (sens) in the developing R2,5 precursors to block ectopic R8 differentiation. Our results support a new model for R8 selection in which lateral inhibition establishes a transient pattern of selected R8s that is permanently reinforced by a repressive bistable loop between sens and ro. This model provides new insight into the strategies that allow successful integration of a repressive patterning signal, such as lateral inhibition, with continued developmental plasticity during retinal differentiation.
机译:感觉器官的模式需要神经诱导和抑制的精确调节。成年果蝇复眼的神经晶体模式是通过为每只单元眼或邻眼单眼选择单个创始人光感受器(R8)生成的。 R8的选择需要一种机制,以将R8的潜力限制在表达前神经基因无声(ato)的一组细胞中的单个细胞中。 R8选择的一种模型表明,R8前体是通过同源域转录因子Rough(Ro)抑制ato从三细胞“ R8等价基团”中选择的。第二种模型提出,侧向抑制足以从称为中间组(IG)的等价细胞组中选择单个R8。在这里,我们提供了新的证据,即对单个R8前体的初始选择需要横向抑制而不是ro。我们显示在ro突变体中,异位R8从R2,5感光受体前体发展而来,与异位Ato无关,并且在指定正常R8s后数小时。我们还显示,Ro直接抑制发展中的R2,5前体中的R8特异性锌指转录因子无意义(sens),以阻止异位R8分化。我们的研究结果支持了R8选择的新模型,其中侧向抑制建立了选定R8的瞬态模式,该模式通过sens和ro之间的抑制性双稳态环永久增强。该模型提供了对策略的新见解,这些策略可以成功整合诸如侧面抑制之类的抑制性模式信号以及视网膜分化过程中持续的发育可塑性。

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