首页> 美国卫生研究院文献>other >The Drosophila T-box transcription factor Midline functions within the Notch–Delta signaling pathway to specify sensory organ precursor cell fates and regulates cell survival within the eye imaginal disc
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The Drosophila T-box transcription factor Midline functions within the Notch–Delta signaling pathway to specify sensory organ precursor cell fates and regulates cell survival within the eye imaginal disc

机译:果蝇T-box转录因子中线在Notch-Delta信号通路内发挥功能以指定感觉器官前体细胞的命运并调节眼部视盘内的细胞存活

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摘要

We report that the T-box transcription factor Midline (Mid), an evolutionary conserved homolog of the vertebrate Tbx20 protein, functions within the Notch–Delta signaling pathway essential for specifying the fates of sensory organ precursor cells. This complements an established history of research showing that Mid regulates the cell-fate specification of diverse cell types within the developing heart, epidermis and central nervous system. Tbx20 has been detected in diverse neuronal and epithelial cells of embryonic eye tissues in both mice and humans. However, the mechanisms by which either Mid or Tbx20 function to regulate cell-fate specification or other critical aspects of eye development including cell survival have not yet been elucidated. We have also gathered preliminary evidence suggesting that Mid may play an indirect, but vital role in selecting SOP cells within the third-instar larval eye disc by regulating the expression of the proneural gene atonal. During subsequent pupal stages, Mid specifies SOP cell fates as a member of the Notch–Delta signaling hierarchy and is essential for maintaining cell viability within by inhibiting apoptotic pathways. We present several new hypotheses that seek to understand the role of Mid in regulating developmental processes downstream of the Notch receptor that are critical for specifying unique cell fates, patterning the adult eye and maintaining cellular homeostasis during eye disc morphogenesis.
机译:我们报告说,T-box转录因子中线(Mid)是脊椎动物Tbx20蛋白的进化保守同源物,在Notch-Delta信号通路内发挥功能,对指定感觉器官前体细胞的命运至关重要。这补充了已有的研究历史,表明Mid调节着正在发育的心脏,表皮和中枢神经系统内各种细胞类型的细胞命运规范。在小鼠和人类的胚胎眼组织的各种神经元和上皮细胞中都检测到了Tbx20。但是,尚未阐明Mid或Tbx20调节细胞命运规范或眼睛发育的其他关键方面(包括细胞存活)的机制。我们还收集了初步证据表明,Mid可能在第三龄幼虫眼盘内选择SOP细胞中起间接作用,但通过调节前突基因无声子的表达发挥至关重要的作用。在随后的p阶段,Mid将SOP细胞命运指定为Notch-Delta信号传导体系的成员,并且对于通过抑制凋亡途径维持细胞活力至关重要。我们提出了一些新的假设,试图了解Mid在调节Notch受体下游的发育过程中的作用,这些作用对于指定独特的细胞命运,构图成年的眼睛以及在眼盘形态发生过程中保持细胞稳态至关重要。

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