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听觉耳蜗中的分隔式和信号选择性缝隙连接耦合

Compartmentalized and signal-selective gap junctional coupling in the hearing cochlea.

作者信息

Jagger Daniel J, Forge Andrew

机构信息

Centre for Auditory Research, UCL Ear Institute, University College London, London WC1X 8EE, United Kingdom.

出版信息

J Neurosci. 2006 Jan 25;26(4):1260-8. doi: 10.1523/JNEUROSCI.4278-05.2006.

Abstract

Gap junctional intercellular communication (GJIC) plays a major role in cochlear function. Recent evidence suggests that connexin 26 (Cx26) and Cx30 are the major constituent proteins of cochlear gap junction channels, possibly in a unique heteromeric configuration. We investigated the functional and structural properties of native cochlear gap junctions in rats, from birth to the onset of hearing [postnatal day 12 (P12)]. Confocal immunofluorescence revealed increasing Cx26 and Cx30 expression from P0 to P12. Functional GJIC was assessed by coinjection of Lucifer yellow (LY) and Neurobiotin (NBN) during whole-cell recordings in cochlear slices. At P0, there was restricted dye transfer between supporting cells around outer hair cells. Transfer was more extensive between supporting cells around inner hair cells. At P8, there was extensive transfer of both dyes between all supporting cell types. By P12, LY no longer transferred between the supporting cells immediately adjacent to hair cells but still transferred between more peripheral cells. NBN transferred freely, but it did not transfer between inner and outer pillar cells. Freeze fracture further demonstrated decreasing GJIC between inner and outer pillar cells around the onset of hearing. These data are supportive of the appearance of signal-selective gap junctions around the onset of hearing, with specific properties required to support auditory function. Furthermore, they suggest that separate medial and lateral buffering compartments exist in the hearing cochlea, which are individually dedicated to the homeostasis of inner hair cells and outer hair cells.

摘要

缝隙连接细胞间通讯(GJIC)在耳蜗功能中起主要作用。最近的证据表明,连接蛋白26(Cx26)和Cx30是耳蜗缝隙连接通道的主要组成蛋白,可能以独特的异聚体形式存在。我们研究了从出生到听力开始[出生后第12天(P12)]大鼠耳蜗天然缝隙连接的功能和结构特性。共聚焦免疫荧光显示从P0到P12,Cx26和Cx30表达增加。在耳蜗切片的全细胞记录过程中,通过共注射荧光素黄(LY)和神经生物素(NBN)评估功能性GJIC。在P0时,外毛细胞周围的支持细胞之间染料转移受限。内毛细胞周围的支持细胞之间转移更广泛。在P8时,两种染料在所有支持细胞类型之间广泛转移。到P12时,LY不再在紧邻毛细胞的支持细胞之间转移,但仍在更外围的细胞之间转移。NBN可自由转移,但不在内柱细胞和外柱细胞之间转移。冷冻蚀刻进一步证明在听力开始时内柱细胞和外柱细胞之间的GJIC减少。这些数据支持在听力开始时出现信号选择性缝隙连接,具有支持听觉功能所需的特定特性。此外,它们表明在听力正常的耳蜗中存在单独的内侧和外侧缓冲区室,分别专门用于内毛细胞和外毛细胞的内环境稳定。

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