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用于研究耳蜗抑制的遗传工具。

Genetic tools for studying cochlear inhibition.

作者信息

Slika Eleftheria, Fuchs Paul Albert

机构信息

The Center for Hearing and Balance, Otolaryngology-Head and Neck Surgery, Johns Hopkins, University School of Medicine Baltimore, Baltimore, MD, United States.

出版信息

Front Cell Neurosci. 2024 Mar 15;18:1372948. doi: 10.3389/fncel.2024.1372948. eCollection 2024.

Abstract

Efferent feedback to the mammalian cochlea includes cholinergic medial olivocochlear neurons (MOCs) that release ACh to hyperpolarize and shunt the voltage change that drives electromotility of outer hair cells (OHCs). Via brainstem connectivity, MOCs are activated by sound in a frequency- and intensity-dependent manner, thereby reducing the amplification of cochlear vibration provided by OHC electromotility. Among other roles, this efferent feedback protects the cochlea from acoustic trauma. Lesion studies, as well as a variety of genetic mouse models, support the hypothesis of efferent protection from acoustic trauma. Genetic knockout and gain-of-function knockin of the unique α9α10-containing nicotinic acetylcholine receptor (nAChR) in hair cells show that acoustic protection correlates with the efficacy of cholinergic inhibition of OHCs. This protective effect was replicated by viral transduction of the gain-of-function α9L9'T nAChR into α9-knockout mice. Continued progress with "efferent gene therapy" will require a reliable method for visualizing nAChR expression in cochlear hair cells. To that end, mice expressing HA-tagged α9 or α10 nAChRs were generated using CRISPR technology. This progress will facilitate continued study of the hair cell nAChR as a therapeutic target to prevent hearing loss and potentially to ameliorate associated pathologies such as hyperacusis.

摘要

哺乳动物耳蜗的传出反馈包括胆碱能内侧橄榄耳蜗神经元(MOCs),这些神经元释放乙酰胆碱,使驱动外毛细胞(OHCs)电运动的电压变化超极化并分流。通过脑干连接,MOCs以频率和强度依赖的方式被声音激活,从而减少OHC电运动提供的耳蜗振动放大。除其他作用外,这种传出反馈可保护耳蜗免受声损伤。损伤研究以及各种基因小鼠模型支持传出保护免受声损伤的假说。毛细胞中独特的含α9α10烟碱型乙酰胆碱受体(nAChR)的基因敲除和功能获得性敲入表明,声保护与胆碱能抑制OHCs的功效相关。通过将功能获得性α9L9'T nAChR病毒转导到α9基因敲除小鼠中,复制了这种保护作用。“传出基因治疗”的持续进展将需要一种可靠的方法来可视化耳蜗毛细胞中的nAChR表达。为此,使用CRISPR技术生成了表达HA标签的α9或α10 nAChRs的小鼠。这一进展将有助于继续研究毛细胞nAChR作为预防听力损失以及潜在改善相关病症(如听觉过敏)的治疗靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7764/10978695/82344aa7b8c1/fncel-18-1372948-g001.jpg

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