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https://hdl.handle.net/20.500.14094/90008398
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2024-12-22
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90008398 (fulltext)
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メタデータID
90008398
アクセス権
open access
出版タイプ
Version of Record
タイトル
Nox3-Derived Superoxide in Cochleae Induces Sensorineural Hearing Loss
著者
Mohri, Hiroaki ; Ninoyu, Yuzuru ; Sakaguchi, Hirofumi ; Hirano, Shigeru ; Saito, Naoaki ; Ueyama, Takehiko
著者名
Mohri, Hiroaki
著者名
Ninoyu, Yuzuru
著者名
Sakaguchi, Hirofumi
著者名
Hirano, Shigeru
著者ID
A0754
研究者ID
1000060178499
著者名
Saito, Naoaki
齋藤, 尚亮
サイトウ, ナオアキ
所属機関名
バイオシグナル総合研究センター
著者ID
A1239
研究者ID
1000080346254
KUID
https://kuid-rm-web.ofc.kobe-u.ac.jp/search/detail?systemId=443e05a0c3fc0358520e17560c007669
著者名
Ueyama, Takehiko
上山, 健彦
ウエヤマ, タケヒコ
所属機関名
バイオシグナル総合研究センター
言語
English (英語)
収録物名
Journal of Neuroscience
巻(号)
41(21)
ページ
4716-4731
出版者
Society for Neuroscience
刊行日
2021-05-26
公開日
2021-07-02
抄録
Reactive oxygen species (ROS) produced by NADPH oxidases (Nox) contribute to the development of different types of sensorineural hearing loss (SNHL), a common impairment in humans with no established treatment. Although the essential role of Nox3 in otoconia biosynthesis and its possible involvement in hearing have been reported in rodents, immunohistological methods targeted at detecting Nox3 expression in inner ear cells reveal ambiguous results. Therefore, the mechanism underlying Nox3-dependent SNHL remains unclear and warrants further investigation. We generated Nox3-Cre knock-in mice, in which Nox3 was replaced with Cre recombinase (Cre). Using Nox3-Cre;tdTomato mice of either sex, in which tdTomato is expressed under the control of the Nox3 promoter, we determined Nox3-expressing regions and cell types in the inner ear. Nox3-expressing cells in the cochlea included various types of supporting cells, outer hair cells, inner hair cells, and spiral ganglion neurons. Nox3 expression increased with cisplatin, age, and noise insults. Moreover, increased Nox3 expression in supporting cells and outer hair cells, especially at the basal turn of the cochlea, played essential roles in ROS-related SNHL. The extent of Nox3 involvement in SNHL follows the following order: cisplatin-induced hearing loss > age-related hearing loss > noise-induced hearing loss. Here, on the basis of Nox3-Cre;tdTomato, which can be used as a reporter system (Nox3-Cre(+/−);tdTomato(+/+) and Nox3-Cre(+/+);tdTomato(+/+)), and Nox3-KO (Nox3-Cre(+/+);tdTomato(+/+)) mice, we demonstrate that Nox3 inhibition in the cochlea is a promising strategy for ROS-related SNHL, such as cisplatin-induced HL, age-related HL, and noise-induced HL.
キーワード
age-related hearing loss
drug-induced hearing loss
hearing loss
NADPH oxidase
noise-induced hearing loss
reactive oxygen species
カテゴリ
バイオシグナル総合研究センター
学術雑誌論文
権利
© 2021 Mohri et al.
This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license, which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed
関連情報
DOI
https://doi.org/10.1523/JNEUROSCI.2672-20.2021
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資源タイプ
journal article
eISSN
1529-2401
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