神戸大学附属図書館デジタルアーカイブ
https://hdl.handle.net/20.500.14094/90004386

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メタデータID
90004386
アクセス権
open access
出版タイプ
Version of Record
タイトル
POU4F3 mutation screening in Japanese hearing loss patients: Massively parallel DNA sequencing-based analysis identified novel variants associated with autosomal dominant hearing loss
著者
Kitano, Tomohiro ; Miyagawa, Maiko ; Nishio, Shin-ya ; Moteki, Hideaki ; Oda, Kiyoshi ; Ohyama, Kenji ; Miyazaki, Hiromitsu ; Hidaka, Hiroshi ; Nakamura, Ken-ichi ; Murata, Takaaki ; Matsuoka, Rina ; Ohta, Yoko ; Nishiyama, Nobuhiro ; Kumakawa, Kozo ; Furutate, Sakiko ; Iwasaki, Satoshi ; Yamada, Takechiyo ; Ohta, Yumi ; Uehara, Natsumi ; Noguchi, Yoshihiro ; Usami, Shin-ichi
著者名
Kitano, Tomohiro
著者名
Miyagawa, Maiko
著者名
Nishio, Shin-ya
著者名
Moteki, Hideaki
著者名
Oda, Kiyoshi
著者名
Ohyama, Kenji
著者名
Miyazaki, Hiromitsu
著者名
Hidaka, Hiroshi
著者名
Nakamura, Ken-ichi
著者名
Murata, Takaaki
著者名
Matsuoka, Rina
著者名
Ohta, Yoko
著者名
Nishiyama, Nobuhiro
著者名
Kumakawa, Kozo
著者名
Furutate, Sakiko
著者名
Iwasaki, Satoshi
著者名
Yamada, Takechiyo
著者名
Ohta, Yumi
著者ID
A1562
研究者ID
1000040570502
KUID
https://kuid-rm-web.ofc.kobe-u.ac.jp/search/detail?systemId=231e60717baefa15520e17560c007669
著者名
Uehara, Natsumi
上原, 奈津美
ウエハラ, ナツミ
所属機関名
医学部附属病院
著者名
Noguchi, Yoshihiro
著者名
Usami, Shin-ichi
言語
English (英語)
収録物名
PLoS ONE
巻(号)
12(5)
ページ
e0177636-e0177636
出版者
Public Library of Science
刊行日
2017-05-17
公開日
2017-12-21
抄録
A variant in a transcription factor gene, POU4F3, is responsible for autosomal dominant nonsyndromic hereditary hearing loss, DFNA15. To date, 14 variants, including a whole deletion of POU4F3, have been reported to cause HL in various ethnic groups. In the present study, genetic screening for POU4F3 variants was carried out for a large series of Japanese hearing loss (HL) patients to clarify the prevalence and clinical characteristics of DFNA15 in the Japanese population. Massively parallel DNA sequencing of 68 target candidate genes was utilized in 2,549 unrelated Japanese HL patients (probands) to identify genomic variations responsible for HL. The detailed clinical features in patients with POU4F3 variants were collected from medical charts and analyzed. Novel 12 POU4F3 likely pathogenic variants (six missense variants, three frameshift variants, and three nonsense variants) were successfully identified in 15 probands (2.5%) among 602 families exhibiting autosomal dominant HL, whereas no variants were detected in the other 1,947 probands with autosomal recessive or inheritance pattern unknown HL. To obtain the audiovestibular configuration of the patients harboring POU4F3 variants, we collected audiograms and vestibular symptoms of the probands and their affected family members. Audiovestibular phenotypes in a total of 24 individuals from the 15 families possessing variants were characterized by progressive HL, with a large variation in the onset age and severity with or without vestibular symptoms observed. Pure-tone audiograms indicated the most prevalent configuration as mid-frequency HL type followed by high-frequency HL type, with asymmetry observed in approximately 20% of affected individuals. Analysis of the relationship between age and pure-tone average suggested that individuals with truncating variants showed earlier onset and slower progression of HL than did those with non-truncating variants. The present study showed that variants in POU4F3 were a common cause of autosomal dominant HL.
カテゴリ
医学部附属病院
学術雑誌論文
権利
© 2017 Kitano et al.
CC license
This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
関連情報
DOI
https://doi.org/10.1371/journal.pone.0177636