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Retracted: A cell cycle‐dependent co‐repressor mediates photoreceptor cell‐specific nuclear receptor function
Author(s) -
Takezawa Shinichiro,
Yokoyama Atsushi,
Okada Maiko,
Fujiki Ryoji,
Iriyama Aya,
Yanagi Yasuo,
Ito Hiroaki,
Takada Ichiro,
Kishimoto Masahiko,
Miyajima Atsushi,
Takeyama Kenichi,
Umesono Kazuhiko,
Kitagawa Hirochika,
Kato Shigeaki
Publication year - 2007
Publication title -
the embo journal
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 7.484
H-Index - 392
eISSN - 1460-2075
pISSN - 0261-4189
DOI - 10.1038/sj.emboj.7601548
Subject(s) - library science , computer science
Photoreceptor cell‐specific nuclear receptor (PNR) (NR2E3) acts as a sequence‐specific repressor that controls neuronal differentiation in the developing retina. We identified a novel PNR co‐repressor, Ret‐CoR, that is expressed in the developing retina and brain. Biochemical purification of Ret‐CoR identified a multiprotein complex that included E2F/Myb‐associated proteins, histone deacetylases (HDACs) and NCoR/HDAC complex‐related components. Ret‐CoR appeared to function as a platform protein for the complex, and interacted with PNR via two CoRNR motifs. Purified Ret‐CoR complex exhibited HDAC activity, co‐repressed PNR transrepression function in vitro , and co‐repressed PNR function in PNR target gene promoters, presumably in the retinal progenitor cells. Notably, the appearance of Ret‐CoR protein was cell‐cycle‐stage‐dependent (from G1 to S). Therefore, Ret‐CoR appears to act as a component of an HDAC co‐repressor complex that supports PNR repression function in the developing retina, and may represent a co‐regulator class that supports transcriptional regulator function via cell‐cycle‐dependent expression.

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