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https://hdl.handle.net/20.500.14094/90004776

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メタデータID
90004776
アクセス権
open access
出版タイプ
Version of Record
タイトル
Antitumor effects of the antiparasitic agent ivermectin via inhibition of Yes-associated protein 1 expression in gastric cancer
著者
Nambara, Sho ; Masuda, Takaaki ; Nishio, Miki ; Kuramitsu, Shotaro ; Tobo, Taro ; Ogawa, Yushi ; Hu, Qingjiang ; Iguchi, Tomohiro ; Kuroda, Yousuke ; Ito, Shuhei ; Eguchi, Hidetoshi ; Sugimachi, Keishi ; Saeki, Hiroshi ; Oki, Eiji ; Maehara, Yoshihiko ; Suzuki, Akira ; Mimori, Koshi
著者名
Nambara, Sho
著者名
Masuda, Takaaki
著者ID
A1704
研究者ID
1000010467897
KUID
https://kuid-rm-web.ofc.kobe-u.ac.jp/search/detail?systemId=b7a90f99283292d1520e17560c007669
著者名
Nishio, Miki
西尾, 美希
ニシオ, ミキ
所属機関名
医学研究科
著者名
Kuramitsu, Shotaro
著者名
Tobo, Taro
著者名
Ogawa, Yushi
著者名
Hu, Qingjiang
著者名
Iguchi, Tomohiro
著者名
Kuroda, Yousuke
著者名
Ito, Shuhei
著者名
Eguchi, Hidetoshi
著者名
Sugimachi, Keishi
著者名
Saeki, Hiroshi
著者名
Oki, Eiji
著者名
Maehara, Yoshihiko
著者ID
A0079
研究者ID
1000010311565
KUID
https://kuid-rm-web.ofc.kobe-u.ac.jp/search/detail?systemId=8e54b581292cf116520e17560c007669
著者名
Suzuki, Akira
鈴木, 聡
スズキ, アキラ
所属機関名
医学研究科
著者名
Mimori, Koshi
言語
English (英語)
収録物名
Oncotarget
巻(号)
8(64)
ページ
107666-107677
出版者
Impact Journals
刊行日
2017-12-08
公開日
2018-04-10
抄録
Yes-associated protein 1 (YAP1) acts as an oncogene through dephosphorylation and nuclear translocation, and nuclear accumulation of YAP1 is associated with poor prognosis in gastric cancer (GC). We previously identified ivermectin, an antiparasitic drug, as a YAP1 inhibitor. Here, we aimed to clarify whether ivermectin had antitumor effects on GC through inhibition of YAP1. First, we evaluated the antiproliferative effects of ivermectin on human GC cells using in vitro proliferation assays and a xenograft mouse model. YAP1-knockdown assays were performed to assess whether the sensitivity to ivermectin depended on YAP1 expression. Next, we explored the mechanism through which ivermectin regulated YAP1 expression or localization by immunoblotting and reverse transcription-quantitative polymerase chain reaction for YAP1 and the downstream gene CTGF. Finally, the clinical significance of YAP1 expression was examined using three independent GC datasets. We found that MKN1 GC cells were most sensitive to ivermectin, whereas MKN7 cells were most resistant. In MKN1 xenografts, ivermectin suppressed tumor growth, and the sensitivity of MKN1 cells to ivermectin was decreased by YAP1 knockdown. Ivermectin inhibited YAP1 nuclear expression and CTGF expression in MKN1 cells but not MKN7 cells. Moreover, ivermectin decreased YAP1 mRNA expression, thereby inhibiting nuclear accumulation of YAP1 in MKN1 cells. In survival analysis, low YAP1 mRNA expression was associated with a better prognosis in three independent GC datasets. In conclusion, we identified ivermectin as a potential antitumor agent and found a promising novel therapeutic strategy for inhibition of GC progression by blocking YAP1 expression.
キーワード
ivermectin
yes-associated protein 1 inhibitor
gastric cancer
antiproliferative effect
therapeutic target
カテゴリ
医学研究科
学術雑誌論文
権利
Nambara et al.
CC license
This is an open-access article distributed under the terms of the Creative Commons Attribution License 3.0 (CC BY 3.0), 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/10.18632/oncotarget.22587