Author:
Rieder Leila E.,Koreski Kaitlin P.,Boltz Kara A.,Kuzu Guray,Urban Jennifer A.,Bowman Sarah K.,Zeidman Anna,Jordan William T.,Tolstorukov Michael Y.,Marzluff William F.,Duronio Robert J.,Larschan Erica N.
Abstract
The conserved histone locus body (HLB) assembles prior to zygotic gene activation early during development and concentrates factors into a nuclear domain of coordinated histone gene regulation. Although HLBs form specifically at replication-dependent histone loci, the cis and trans factors that target HLB components to histone genes remained unknown. Here we report that conserved GA repeat cis elements within the bidirectional histone3–histone4 promoter direct HLB formation in Drosophila. In addition, the CLAMP (chromatin-linked adaptor for male-specific lethal [MSL] proteins) zinc finger protein binds these GA repeat motifs, increases chromatin accessibility, enhances histone gene transcription, and promotes HLB formation. We demonstrated previously that CLAMP also promotes the formation of another domain of coordinated gene regulation: the dosage-compensated male X chromosome. Therefore, CLAMP binding to GA repeat motifs promotes the formation of two distinct domains of coordinated gene activation located at different places in the genome.
Funder
National Institutes of Health
NIH
American Cancer Society
Pew Biomedical Scholars
Publisher
Cold Spring Harbor Laboratory
Subject
Developmental Biology,Genetics
Cited by
50 articles.
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