the role of histone methylation and h2a.z occupancy during rapid activation of ethylene responsive genes组蛋白甲基化和h2a的角色。.pdfVIP
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the role of histone methylation and h2a.z occupancy during rapid activation of ethylene responsive genes组蛋白甲基化和h2a的角色。
The Role of Histone Methylation and H2A.Z Occupancy
during Rapid Activation of Ethylene Responsive Genes
Yongfeng Hu, Yuan Shen, Natalia Conde e Silva, Dao-Xiu Zhou*
´
Institut de Biologie des Plantes, Universite Paris-Sud, Orsay, France
Abstract
Ethylene signaling pathway leads to rapid gene activation by two hierarchies of transcription factors with EIN3/EIL proteins
as primary ones and ERF proteins as secondary ones. The role of chromatin modifications during the rapid gene activation is
not known. In this work we studied trimethylated histone H3 lysine 4 (H3K4me3) and lysine 27 (H3K27me3), two opposite
histone methylation marks for gene activity, during the induction course of three ethylene-responsive genes (ERF1, AtERF14
and ChiB). We found that the three genes displayed different histone modification profiles before induction. After induction,
H3K4me3 was increased in the 59 region and the gene body of ERF1, while H3K27me3 was decreased in the promoter of
AtERF14. But the modification changes were later than the gene activation. Analysis of other rapidly inducible ERF genes
confirmed the observation. In addition, histone H2A.Z occupancy on the three genes and the association of the H3K27me3-
binding protein LHP1 with AtERF14 and ChiB were not affected by the inductive signal. However, the mutation of genes
encoding H2A.Z and LHP1 attenuated and enhanced respectively the induction of target genes and altered H3K4me3.
These results indicate that the induction of ethylene-responsive genes does not require immediate modulation of H3K4me3
and H3K27me3 and dissociation of LHP1 and H2A.Z from the targets, and suggest that the chromatin structure of the genes
before induction is committed for transcriptional activation and that H3K4me3 is not required for ethylene-responsive gene
activation, but may serve as a mark for
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