CLOCK, an essential pacemaker component, controls expression of the circadian transcription factor DBP
- 1Département de Biologie Moléculaire, Science II, Université de Genève, CH-1211 Genève 4, Switzerland; 2Laboratory of Developmental Chronobiology, Pediatric Service, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts 02114 USA; 3Program in Neuroscience, Harvard Medical School, Boston, Massachusetts 02115 USA
Abstract
DBP, the founding member of the PAR leucine zipper transcription factor family, is expressed according to a robust daily rhythm in the suprachiasmatic nucleus and several peripheral tissues. Previous studies with mice deleted for the Dbp gene have established that DBP participates in the regulation of several clock outputs, including locomotor activity, sleep distribution, and liver gene expression. Here we present evidence that circadian Dbptranscription requires the basic helix–loop–helix–PAS protein CLOCK, an essential component of the negative-feedback circuitry generating circadian oscillations in mammals and fruit flies. Genetic and biochemical experiments suggest that CLOCK regulates Dbpexpression by binding to E-box motifs within putative enhancer regions located in the first and second introns. Similar E-box motifs have been found previously in the promoter sequence of the murine clock genemPeriod1. Hence, the same molecular mechanisms generating circadian oscillations in the expression of clock genes may directly control the rhythmic transcription of clock output regulators such asDbp.
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Footnotes
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↵4 Corresponding author.
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E-MAIL ueli.schibler{at}molbio.unige.ch; FAX 41 22 702 68 68.
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- Received December 3, 1999.
- Accepted January 31, 2000.
- Cold Spring Harbor Laboratory Press
