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Zebrafish dou yan Mutation Causes Patterning Defects and Extensive Cell Death in the Retina

机译:斑马鱼dou yan突变导致图案缺陷和视网膜广泛的细胞死亡。

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摘要

The size of an organ is largely determined by the number of cells it contains, which in turn is regulated by two opposing processes: cell proliferation and cell death, but it is generally not clear how cell proliferation and cell death are coordinated during development. Here we characterize the zebrafish dou yanmi234 mutation that results in a dramatic reduction of retinal size and a disruption of retinal differentiation and lamination. The retinal size reduction is caused by increased retinal cell death in a non-cell-autonomous manner during early development. The phenotypic defect in dou yanmi234 arises coincident with the onset of retinal neurogenesis and differentiation. Interestingly, unlike many other small eye mutations, the mutation does not increase the level of cell death in the brain, implying the brain and retina utilize different mechanisms to maintain cell survival. Identification and further study of the dou yan gene will enhance our understanding of the molecular mechanisms regulating retinal cellular homeostasis, i.e. the balance between cell proliferation and cell death.
机译:器官的大小在很大程度上取决于它所包含的细胞数量,而细胞的数量又由两个相反的过程调节:细胞增殖和细胞死亡,但是通常不清楚在发育过程中如何协调细胞增殖和细胞死亡。在这里,我们描述了斑马鱼dou yan mi234 突变的特征,该突变导致视网膜大小显着减小以及视网膜分化和覆膜破坏。视网膜大小的减少是由早期发育过程中以非细胞自主方式增加的视网膜细胞死亡引起的。 dou yan mi234 的表型缺陷与视网膜神经发生和分化的发生同时发生。有趣的是,与许多其他小眼突变不同,该突变不会增加大脑中细胞的死亡水平,这意味着大脑和视网膜利用不同的机制来维持细胞存活。 dou yan基因的鉴定和进一步研究将增进我们对调节视网膜细胞稳态的分子机制的理解,即细胞增殖与细胞死亡之间的平衡。

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