deposition of histone variant h2a.z within gene bodies regulates responsive genesh2a沉积的组蛋白变体。.pdfVIP
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deposition of histone variant h2a.z within gene bodies regulates responsive genesh2a沉积的组蛋白变体。
Deposition of Histone Variant H2A.Z within Gene Bodies
Regulates Responsive Genes
Devin Coleman-Derr, Daniel Zilberman*
Department of Plant and Microbial Biology, University of California Berkeley, Berkeley, California, United States of America
Abstract
The regulation of eukaryotic chromatin relies on interactions between many epigenetic factors, including histone
modifications, DNA methylation, and the incorporation of histone variants. H2A.Z, one of the most conserved but enigmatic
histone variants that is enriched at the transcriptional start sites of genes, has been implicated in a variety of chromosomal
processes. Recently, we reported a genome-wide anticorrelation between H2A.Z and DNA methylation, an epigenetic
hallmark of heterochromatin that has also been found in the bodies of active genes in plants and animals. Here, we
investigate the basis of this anticorrelation using a novel h2a.z loss-of-function line in Arabidopsis thaliana. Through
genome-wide bisulfite sequencing, we demonstrate that loss of H2A.Z in Arabidopsis has only a minor effect on the level or
profile of DNA methylation in genes, and we propose that the global anticorrelation between DNA methylation and H2A.Z is
primarily caused by the exclusion of H2A.Z from methylated DNA. RNA sequencing and genomic mapping of H2A.Z show
that H2A.Z enrichment across gene bodies, rather than at the TSS, is correlated with lower transcription levels and higher
measures of gene responsiveness. Loss of H2A.Z causes misregulation of many genes that are disproportionately associated
with response to environmental and developmental stimuli. We propose that H2A.Z deposition in gene bodies promotes
variability in levels and patterns of gene expression, and that a major function of genic DNA methylation is to exclude H2A.Z
fro
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