CREB Binds to Multiple Loci on Human Chromosome 22

Author:

Euskirchen Ghia1,Royce Thomas E.2,Bertone Paul1,Martone Rebecca1,Rinn John L.2,Nelson F. Kenneth1,Sayward Fred3,Luscombe Nicholas M.2,Miller Perry3,Gerstein Mark2,Weissman Sherman4,Snyder Michael12

Affiliation:

1. Department of Molecular, Cellular and Developmental Biology

2. Department of Molecular Biophysics and Biochemistry

3. Department of Medical Anesthesiology

4. Department of Genetics, Yale University, New Haven, Connecticut 06520-8005

Abstract

ABSTRACT The cyclic AMP-responsive element-binding protein (CREB) is an important transcription factor that can be activated by hormonal stimulation and regulates neuronal function and development. An unbiased, global analysis of where CREB binds has not been performed. We have mapped for the first time the binding distribution of CREB along an entire human chromosome. Chromatin immunoprecipitation of CREB-associated DNA and subsequent hybridization of the associated DNA to a genomic DNA microarray containing all of the nonrepetitive DNA of human chromosome 22 revealed 215 binding sites corresponding to 192 different loci and 100 annotated potential gene targets. We found binding near or within many genes involved in signal transduction and neuronal function. We also found that only a small fraction of CREB binding sites lay near well-defined 5′ ends of genes; the majority of sites were found elsewhere, including introns and unannotated regions. Several of the latter lay near novel unannotated transcriptionally active regions. Few CREB targets were found near full-length cyclic AMP response element sites; the majority contained shorter versions or close matches to this sequence. Several of the CREB targets were altered in their expression by treatment with forskolin; interestingly, both induced and repressed genes were found. Our results provide novel molecular insights into how CREB mediates its functions in humans.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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