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タイトル: Enhancement of Vivid-based photo-activatable Gal4 transcription factor in mammalian cells
著者: Nagasaki, Shinji C.
Fukuda, Tomonori D.
Yamada, Mayumi  kyouindb  KAKEN_id  orcid https://orcid.org/0000-0001-6272-3704 (unconfirmed)
Suzuki, Yusuke III
Kakutani, Ryo
Guy, Adam T.
Imayoshi, Itaru  kyouindb  KAKEN_id  orcid https://orcid.org/0000-0001-9728-481X (unconfirmed)
著者名の別形: 長崎, 真治
福田, 智徳
山田, 真弓
鈴木, 裕輔
角谷, 亮
今吉, 格
キーワード: optogenetics
Gal4/UAS system
transcription
gene expression
Vivid
発行日: 2023
出版者: Japan Society for Cell Biology
誌名: Cell Structure and Function
巻: 48
号: 1
開始ページ: 31
終了ページ: 47
抄録: The Gal4/UAS system is a versatile tool to manipulate exogenous gene expression of cells spatially and temporally in many model organisms. Many variations of light-controllable Gal4/UAS system are now available, following the development of photo-activatable (PA) molecular switches and integration of these tools. However, many PA-Gal4 transcription factors have undesired background transcription activities even in dark conditions, and this severely attenuates reliable light-controlled gene expression. Therefore, it is important to develop reliable PA-Gal4 transcription factors with robust light-induced gene expression and limited background activity. By optimization of synthetic PA-Gal4 transcription factors, we have validated configurations of Gal4 DNA biding domain, transcription activation domain and blue light-dependent dimer formation molecule Vivid (VVD), and applied types of transcription activation domains to develop a new PA-Gal4 transcription factor we have named eGAV (enhanced Gal4-VVD transcription factor). Background activity of eGAV in dark conditions was significantly lower than that of hGAVPO, a commonly used PA-Gal4 transcription factor, and maximum light-induced gene expression levels were also improved. Light-controlled gene expression was verified in cultured HEK293T cells with plasmid-transient transfections, and in mouse EpH4 cells with lentivirus vector-mediated transduction. Furthermore, light-controlled eGAV-mediated transcription was confirmed in transfected neural stem cells and progenitors in developing and adult mouse brain and chick spinal cord, and in adult mouse hepatocytes, demonstrating that eGAV can be applied to a wide range of experimental systems and model organisms.
著作権等: Copyright: ©2023 The Author(s).
This is an open access article distributed under the terms of the Creative Commons BY (Attribution) License, which permits the unrestricted distribution, reproduction and use of the article provided the original source and authors are credited.
URI: http://hdl.handle.net/2433/286502
DOI(出版社版): 10.1247/csf.22074
PubMed ID: 36529516
出現コレクション:学術雑誌掲載論文等

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