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TBX1 对于正常的血管纹和半规管发育是必需的。

TBX1 is required for normal stria vascularis and semicircular canal development.

机构信息

The Jackson Laboratory, Bar Harbor, ME, 04609, USA.

The Jackson Laboratory, Bar Harbor, ME, 04609, USA.

出版信息

Dev Biol. 2020 Jan 1;457(1):91-103. doi: 10.1016/j.ydbio.2019.09.013. Epub 2019 Sep 21.

Abstract

Little is known about the role of TBX1 in post-otocyst stages of inner ear development. Here, we report on mice with a missense mutation of Tbx1 that are viable with fully developed but abnormally formed inner ears. Mutant mice are deaf due to an undeveloped stria vascularis and show vestibular dysfunction associated with abnormal semicircular canal formation. We show that TBX1 is expressed in endolymph-producing strial marginal cells and vestibular dark cells of the inner ear and is an upstream regulator of Esrrb, which previously was shown to control the developmental fate of these cells. We also show that TBX1 is expressed in sensory cells of the crista ampullaris, which may relate to the semicircular canal abnormalities observed in mutant mice. Inner ears of mutant embryos have a non-resorbed fusion plate in the posterior semicircular canal and a single ampulla connecting anterior and lateral canals. We hypothesize that the TBX1 missense mutation prevents binding with specific co-regulatory proteins. These findings reveal previously unknown functions of TBX1 during later stages of inner ear development.

摘要

关于 Tbx1 在内耳后卵囊发育阶段的作用知之甚少。在这里,我们报告了 Tbx1 错义突变的小鼠具有完全发育但异常形成的内耳,且是存活的。由于纹状血管发育不全,突变小鼠失聪,并表现出与半规管异常形成相关的前庭功能障碍。我们表明 TBX1 在产生内淋巴的边缘细胞和内耳的前庭暗细胞中表达,是 Esrrb 的上游调节剂,先前的研究表明 Esrrb 控制这些细胞的发育命运。我们还表明,TBX1 在壶腹嵴的感觉细胞中表达,这可能与突变小鼠中观察到的半规管异常有关。突变胚胎的内耳在后半规管中有一个未吸收的融合板,以及一个连接前和侧管的单个壶腹。我们假设 TBX1 错义突变阻止了与特定的共调节蛋白结合。这些发现揭示了 TBX1 在内耳发育后期的未知功能。

相似文献

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TBX1 is required for inner ear morphogenesis.内耳形态发生需要TBX1。
Hum Mol Genet. 2003 Aug 15;12(16):2041-8. doi: 10.1093/hmg/ddg216.

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