System-level identification of transcriptional circuits underlying mammalian circadian clocks

被引:0
|
作者
Hiroki R Ueda
Satoko Hayashi
Wenbin Chen
Motoaki Sano
Masayuki Machida
Yasufumi Shigeyoshi
Masamitsu Iino
Seiichi Hashimoto
机构
[1] Molecular Medicine Laboratories,Department of Pharmacology
[2] Institute for Drug Discovery Research,Department of Anatomy and Neurobiology
[3] Yamanouchi Pharmaceutical Co.,undefined
[4] Ltd.,undefined
[5] 21 Miyukigaoka,undefined
[6] Tsukuba,undefined
[7] Laboratory for Systems Biology,undefined
[8] Center for Developmental Biology,undefined
[9] RIKEN,undefined
[10] 2-2-3 Minatojima-minamimachi,undefined
[11] Chuo-ku,undefined
[12] Graduate School of Medicine,undefined
[13] The University of Tokyo,undefined
[14] 7-3-1 Bunkyo-ku,undefined
[15] Research Center for Glycoscience,undefined
[16] National Institute of Advanced Industrial Science and Technology,undefined
[17] Central 6,undefined
[18] 1-1,undefined
[19] Higashi,undefined
[20] Tsukuba,undefined
[21] Kinki University School of Medicine,undefined
[22] 377-2 Ohno-Higashi,undefined
来源
Nature Genetics | 2005年 / 37卷
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摘要
Mammalian circadian clocks consist of complexly integrated regulatory loops1,2,3,4,5, making it difficult to elucidate them without both the accurate measurement of system dynamics and the comprehensive identification of network circuits6. Toward a system-level understanding of this transcriptional circuitry, we identified clock-controlled elements on 16 clock and clock-controlled genes in a comprehensive surveillance of evolutionarily conserved cis elements and measurement of their transcriptional dynamics. Here we report the roles of E/E′ boxes, DBP/E4BP4 binding elements7 and RevErbA/ROR binding elements8 in nine, seven and six genes, respectively. Our results indicate that circadian transcriptional circuits are governed by two design principles: regulation of E/E′ boxes and RevErbA/ROR binding elements follows a repressor-precedes-activator pattern, resulting in delayed transcriptional activity, whereas regulation of DBP/E4BP4 binding elements follows a repressor-antiphasic-to-activator mechanism, which generates high-amplitude transcriptional activity. Our analysis further suggests that regulation of E/E′ boxes is a topological vulnerability in mammalian circadian clocks, a concept that has been functionally verified using in vitro phenotype assay systems.
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页码:187 / 192
页数:5
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