Reciprocal regulation of haem biosynthesis and the circadian clock in mammals

被引:0
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作者
Krista Kaasik
Cheng Chi Lee
机构
[1] Baylor College of Medicine,Department of Molecular and Human Genetics
[2] Tartu University,Department of Biotechnology, Institute of Molecular and Cell Biology
[3] University of Texas Health Science Center,Department of Biochemistry and Molecular Biology
来源
Nature | 2004年 / 430卷
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摘要
The circadian clock is the central timing system that controls numerous physiological processes. In mammals, one such process is haem biosynthesis, which the clock controls through regulation of the rate-limiting enzyme aminolevulinate synthase 1 (Alas1)1,2. Several members of the core clock mechanism are PAS domain proteins, one of which, neuronal PAS 2 (NPAS2), has a haem-binding motif3,4. Indeed, haem controls activity of the BMAL1–NPAS2 transcription complex in vitro by inhibiting DNA binding in response to carbon monoxide3. Here we show that haem differentially modulates expression of the mammalian Period genes mPer1 and mPer2in vivo by a mechanism involving NPAS2 and mPER2. Further experiments show that mPER2 positively stimulates activity of the BMAL1–NPAS2 transcription complex and, in turn, NPAS2 transcriptionally regulates Alas1. Vitamin B12 and haem compete for binding to NPAS2 and mPER2, but they have opposite effects on mPer2 and mPer1 expression in vivo. Our data show that the circadian clock and haem biosynthesis are reciprocally regulated and suggest that porphyrin-containing molecules are potential targets for therapy of circadian disorders.
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页码:467 / 471
页数:4
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