Analysis and synthesis of high-amplitude Cis -elements in the mammalian circadian clock
Author(s) -
Yuichi Kumaki,
Maki UkaiTadenuma,
Kenichiro D. Uno,
Junko Nishio,
Kohhei Masumoto,
Mamoru Nagano,
Takashi Komori,
Yasufumi Shigeyoshi,
John B. Hogenesch,
Hiroki R. Ueda
Publication year - 2008
Publication title -
proceedings of the national academy of sciences
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.011
H-Index - 771
eISSN - 1091-6490
pISSN - 0027-8424
DOI - 10.1073/pnas.0802636105
Subject(s) - circadian clock , enhancer , clock network , circadian rhythm , computational biology , biology , transcriptional regulation , microbiology and biotechnology , gene , genetics , computer science , gene expression , neuroscience , synchronous circuit , clock signal , telecommunications , jitter
Mammalian circadian clocks consist of regulatory loops mediated by Clock/Bmal1-binding elements, DBP/E4BP4 binding elements, and RevErbA/ROR binding elements. As a step toward system-level understanding of the dynamic transcriptional regulation of the oscillator, we constructed and used a mammalian promoter/enhancer database (http://promoter.cdb.riken.jp/) with computational models of the Clock/Bmal1-binding elements, DBP/E4BP4 binding elements, and RevErbA/ROR binding elements to predict new targets of the clock and subsequently validated these targets at the level of the cell and organism. We further demonstrated the predictive nature of these models by generating and testing synthetic regulatory elements that do not occur in nature and showed that these elements produced high-amplitude circadian gene regulation. Biochemical experiments to characterize these synthetic elements revealed the importance of the affinity balance between transactivators and transrepressors in generating high-amplitude circadian transcriptional output. These results highlight the power of comparative genomics approaches for system-level identification and knowledge-based design of dynamic regulatory circuits.
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