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Article

Regulation of Gene Transcription by the Histone H2A N-Terminal Domain

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Pages 7641-7648 | Received 27 Apr 2007, Accepted 13 Aug 2007, Published online: 27 Mar 2023
 

Abstract

Histone N-terminal domains play critical roles in regulating chromatin structure and gene transcription. Relatively little is known, however, about the role of the histone H2A N-terminal domain in transcription regulation. We have used DNA microarrays to characterize the changes in genome-wide expression caused by mutations in the N-terminal domain of histone H2A. Our results indicate that the N-terminal domain of histone H2A functions primarily to repress the transcription of a large subset of the Saccharomyces cerevisiae genome and that most of the H2A-repressed genes are also repressed by the histone H2B N-terminal domain. Using the histone H2A microarray data, we selected three reporter genes (BNA1, BNA2, and GCY1), which we subsequently used to map regions in the H2A N-terminal domain responsible for this transcriptional repression. These studies revealed that a small subdomain in the H2A N-terminal tail, comprised of residues 16 to 20, is required for the transcriptional repression of these reporter genes. Deletion of either the entire histone H2A N-terminal domain or just this small subdomain imparts sensitivity to UV irradiation. Finally, we show that two residues in this H2A subdomain, serine-17 and arginine-18, are specifically required for the transcriptional repression of the BNA2 reporter gene.

SUPPLEMENTAL MATERIAL

We are grateful to Deirdre Fahy, Lisa Gloss, Yi Jin, McKenna Kyriss, Ray Reeves, and Julie Stanton for helpful discussions and comments on the manuscript.

This work was supported by American Cancer Society grant RSG-03-181-01-GMC.

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