Notch 配体 Jagged1 对于小鼠耳蜗中 Hen-sen 细胞的形成、维持和存活是必需的。
The Notch Ligand Jagged1 Is Required for the Formation, Maintenance, and Survival of Hensen's Cells in the Mouse Cochlea.
机构信息
Solomon H. Snyder Department of Neuroscience and.
Departments of Pharmacology.
出版信息
J Neurosci. 2020 Dec 2;40(49):9401-9413. doi: 10.1523/JNEUROSCI.1192-20.2020. Epub 2020 Oct 30.
During cochlear development, the Notch ligand JAGGED 1 (JAG1) plays an important role in the specification of the prosensory region, which gives rise to sound-sensing hair cells and neighboring supporting cells (SCs). While JAG1's expression is maintained in SCs through adulthood, the function of JAG1 in SC development is unknown. Here, we demonstrate that JAG1 is essential for the formation and maintenance of Hensen's cells, a highly specialized SC subtype located at the edge of the auditory epithelium. Using :: mice of both genders, we show that deletion at the onset of differentiation, at embryonic day 14.5, disrupted Hensen's cell formation. Similar loss of Hensen's cells was observed when was deleted after Hensen's cell formation at postnatal day (P) 0/P1 and fate-mapping analysis revealed that in the absence of , some Hensen's cells die, but others convert into neighboring Claudius cells. In support of a role for JAG1 in cell survival, genes involved in mitochondrial function and protein synthesis were downregulated in the sensory epithelium of P0 cochlea lacking Finally, using :: mice to delete at P0, we observed a similar loss of Hensen's cells and found that adult mutant mice have hearing deficits at the low-frequency range. Hensen's cells play an essential role in the development and homeostasis of the cochlea. Defects in the biophysical or functional properties of Hensen's cells have been linked to auditory dysfunction and hearing loss. Despite their importance, surprisingly little is known about the molecular mechanisms that guide their development. Morphologic and fate-mapping analyses in our study revealed that, in the absence of the Notch ligand JAGGED1, Hensen's cells died or converted into Claudius cells, which are specialized epithelium-like cells outside the sensory epithelium. Confirming a link between JAGGED1 and cell survival, transcriptional profiling showed that JAGGED1 maintains genes critical for mitochondrial function and tissue homeostasis. Finally, auditory phenotyping revealed that JAGGED1's function in supporting cells is necessary for low-frequency hearing.
在耳蜗发育过程中,Notch 配体 JAGGED 1(JAG1)在原感受区域的特化中发挥重要作用,该区域产生感受声音的毛细胞和相邻的支持细胞(SCs)。虽然 JAG1 的表达在成年 SC 中得以维持,但 JAG1 在 SC 发育中的功能尚不清楚。在这里,我们证明 JAG1 对于高度特化的支持细胞亚型——Hensen 细胞的形成和维持是必不可少的,Hensen 细胞位于听觉上皮的边缘。我们使用两种性别的 :: 小鼠,显示出在胚胎第 14.5 天分化开始时删除 会破坏 Hensen 细胞的形成。当在出生后第 0/1 天(P)Hensen 细胞形成后删除 时,观察到类似的 Hensen 细胞缺失,并且命运图谱分析显示,在没有 的情况下,一些 Hensen 细胞死亡,但其他细胞转化为相邻的 Claudius 细胞。支持 JAG1 在细胞存活中的作用,涉及线粒体功能和蛋白质合成的基因在缺乏 的 P0 耳蜗感觉上皮中下调。最后,使用 :: 小鼠在 P0 时删除 ,我们观察到类似的 Hensen 细胞缺失,并发现成年 突变小鼠在低频范围内存在听力缺陷。Hensen 细胞在耳蜗的发育和稳态中起着至关重要的作用。Hensen 细胞的生物物理或功能特性缺陷与听觉功能障碍和听力损失有关。尽管它们很重要,但令人惊讶的是,人们对指导其发育的分子机制知之甚少。在我们的研究中,形态学和命运图谱分析显示,在缺乏 Notch 配体 JAGGED1 的情况下,Hensen 细胞死亡或转化为 Claudius 细胞,Claudius 细胞是位于感觉上皮外的特化上皮样细胞。转录谱分析证实了 JAGGED1 与细胞存活之间的联系,表明 JAGGED1 维持了关键的线粒体功能和组织稳态基因。最后,听觉表型分析显示,JAGGED1 在支持细胞中的功能对于低频听力是必要的。
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