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Onecut1 对于水平细胞的发生和视网膜的完整性是必需的。

Onecut1 is essential for horizontal cell genesis and retinal integrity.

机构信息

Department of Ophthalmology/Ross Eye Institute and Developmental Genomics Group, New York State Center of Excellence in Bioinformatics and Life Sciences, University at Buffalo, Buffalo, New York 14203, USA.

出版信息

J Neurosci. 2013 Aug 7;33(32):13053-65, 13065a. doi: 10.1523/JNEUROSCI.0116-13.2013.

Abstract

Horizontal cells are interneurons that synapse with photoreceptors in the outer retina. Their genesis during development is subject to regulation by transcription factors in a hierarchical manner. Previously, we showed that Onecut 1 (Oc1), an atypical homeodomain transcription factor, is expressed in developing horizontal cells (HCs) and retinal ganglion cells (RGCs) in the mouse retina. Herein, by knocking out Oc1 specifically in the developing retina, we show that the majority (∼80%) of HCs fail to form during early retinal development, implying that Oc1 is essential for HC genesis. However, no other retinal cell types, including RGCs, were affected in the Oc1 knock-out. Analysis of the genetic relationship between Oc1 and other transcription factor genes required for HC development revealed that Oc1 functions downstream of FoxN4, in parallel with Ptf1a, but upstream of Lim1 and Prox1. By in utero electroporation, we found that Oc1 and Ptf1a together are not only essential, but also sufficient for determination of HC fate. In addition, the synaptic connections in the outer plexiform layer are defective in Oc1-null mice, and photoreceptors undergo age-dependent degeneration, indicating that HCs are not only an integral part of the retinal circuitry, but also are essential for the survival of photoreceptors. In sum, these results demonstrate that Oc1 is a critical determinant of HC fate, and reveal that HCs are essential for photoreceptor viability, retinal integrity, and normal visual function.

摘要

水平细胞是与外视网膜中的光感受器形成突触的中间神经元。它们在发育过程中的发生受到转录因子的分层调节。先前,我们表明,一种非典型同源结构域转录因子 Onecut 1(Oc1)在外周视网膜的发育中的水平细胞(HCs)和视网膜神经节细胞(RGCs)中表达。在此,通过在发育中的视网膜中特异性敲除 Oc1,我们表明在早期视网膜发育过程中,大多数(约 80%)HCs 未能形成,这表明 Oc1 对于 HC 发生是必不可少的。然而,Oc1 敲除并没有影响其他视网膜细胞类型,包括 RGCs。对 Oc1 与 HC 发育所需的其他转录因子基因之间的遗传关系进行分析表明,Oc1 作为 FoxN4 的下游分子,与 Ptf1a 平行发挥作用,但在 Lim1 和 Prox1 之前发挥作用。通过在体电穿孔,我们发现 Oc1 和 Ptf1a 一起不仅是必需的,而且对于 HC 命运的确定也是充分的。此外,Oc1 缺失小鼠的外丛状层中的突触连接存在缺陷,光感受器发生年龄依赖性退化,表明 HCs 不仅是视网膜回路的组成部分,而且对于光感受器的存活也是必不可少的。总之,这些结果表明 Oc1 是 HC 命运的关键决定因素,并揭示了 HCs 对于光感受器的存活、视网膜的完整性和正常视觉功能是必不可少的。

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