TY - JOUR
T1 - Genome-wide Expression Analysis of Mouse Liver Reveals CLOCK-regulated Circadian Output Genes
AU - Oishi, Katsutaka
AU - Miyazaki, Koyomi
AU - Kadota, Koji
AU - Kikuno, Reiko
AU - Nagase, Takahiro
AU - Atsumi, Gen Ichi
AU - Ohkura, Naoki
AU - Azama, Takashi
AU - Mesaki, Miho
AU - Yukimasa, Shima
AU - Kobayashi, Hisato
AU - Iitaka, Chisato
AU - Umehara, Takashi
AU - Horikoshi, Masami
AU - Kudo, Takashi
AU - Shimizu, Yoshihisa
AU - Yano, Masahiko
AU - Monden, Morito
AU - Machida, Kazuhiko
AU - Matsuda, Juzo
AU - Horie, Shuichi
AU - Todo, Takeshi
AU - Ishida, Norio
PY - 2003/10/17
Y1 - 2003/10/17
N2 - CLOCK is a positive component of a transcription/ translation-based negative feedback loop of the central circadian oscillator in the suprachiasmatic nucleus in mammals. To examine CLOCK-regulated circadian transcription in peripheral tissues, we performed microarray analyses using liver RNA isolated from Clock mutant mice. We also compared expression profiles with those of Cryptochromes (Cry1 and Cry2) double knockout mice. We identified more than 100 genes that fluctuated from day to night and of which expression levels were decreased in Clock mutant mice. In Cry-deficient mice, the expression levels of most CLOCK-regulated genes were elevated to the upper range of normal oscillation. Most of the screened genes had a CLOCK/BMAL1 binding site (E box) in the 5′-flanking region. We found that CLOCK was absolutely concerned with the circadian transcription of one type of liver genes (such as DBP, TEF, and Usp2) and partially with another (such as mPer1, mPer2, mDec1, Nocturnin, P450 oxidoreductase, and FKBP51) because the latter were damped but remained rhythmic in the mutant mice. Our results showed that CLOCK and CRY proteins are involved in the transcriptional regulation of many circadian output genes in the mouse liver. In addition to being a core component of the negative feedback loop that drives the circadian oscillator, CLOCK also appears to be involved in various physiological functions such as cell cycle, lipid metabolism, immune functions, and proteolysis in peripheral tissues.
AB - CLOCK is a positive component of a transcription/ translation-based negative feedback loop of the central circadian oscillator in the suprachiasmatic nucleus in mammals. To examine CLOCK-regulated circadian transcription in peripheral tissues, we performed microarray analyses using liver RNA isolated from Clock mutant mice. We also compared expression profiles with those of Cryptochromes (Cry1 and Cry2) double knockout mice. We identified more than 100 genes that fluctuated from day to night and of which expression levels were decreased in Clock mutant mice. In Cry-deficient mice, the expression levels of most CLOCK-regulated genes were elevated to the upper range of normal oscillation. Most of the screened genes had a CLOCK/BMAL1 binding site (E box) in the 5′-flanking region. We found that CLOCK was absolutely concerned with the circadian transcription of one type of liver genes (such as DBP, TEF, and Usp2) and partially with another (such as mPer1, mPer2, mDec1, Nocturnin, P450 oxidoreductase, and FKBP51) because the latter were damped but remained rhythmic in the mutant mice. Our results showed that CLOCK and CRY proteins are involved in the transcriptional regulation of many circadian output genes in the mouse liver. In addition to being a core component of the negative feedback loop that drives the circadian oscillator, CLOCK also appears to be involved in various physiological functions such as cell cycle, lipid metabolism, immune functions, and proteolysis in peripheral tissues.
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U2 - 10.1074/jbc.M304564200
DO - 10.1074/jbc.M304564200
M3 - Article
C2 - 12865428
AN - SCOPUS:16744364055
SN - 0021-9258
VL - 278
SP - 41519
EP - 41527
JO - Journal of Biological Chemistry
JF - Journal of Biological Chemistry
IS - 42
ER -