The CHD3 Remodeler PICKLE Promotes Trimethylation of Histone H3 Lysine 27

Zhang, Heng; Rider, S. Dean; Henderson, J.; Fountain, Matthew D.; Chuang, King; Kandachar, Vasundhara; Simons, Alexis; Edenberg, Howard J.; Romero‐Severson, Jeanne; Muir, William M.; Ogas, Joe

doi:10.1074/jbc.m802129200

Cited by 131 publications

(84 citation statements)

References 62 publications

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“…This is consistent with earlier observations by others [23]. Because we failed to detect direct binding of PKL to any of the up-regulated genes, we conclude that increased expression of these genes in pkl is an indirect effect.…”

Section: Discussionsupporting

confidence: 94%

CHD3 Proteins and Polycomb Group Proteins Antagonistically Determine Cell Identity in Arabidopsis

Aichinger¹,

Villar²,

et al. 2009

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Dynamic regulation of chromatin structure is of fundamental importance for modulating genomic activities in higher eukaryotes. The opposing activities of Polycomb group (PcG) and trithorax group (trxG) proteins are part of a chromatin-based cellular memory system ensuring the correct expression of specific transcriptional programs at defined developmental stages. The default silencing activity of PcG proteins is counteracted by trxG proteins that activate PcG target genes and prevent PcG mediated silencing activities. Therefore, the timely expression and regulation of PcG proteins and counteracting trxG proteins is likely to be of fundamental importance for establishing cell identity. Here, we report that the chromodomain/helicase/DNA–binding domain CHD3 proteins PICKLE (PKL) and PICKLE RELATED2 (PKR2) have trxG-like functions in plants and are required for the expression of many genes that are repressed by PcG proteins. The pkl mutant could partly suppress the leaf and flower phenotype of the PcG mutant curly leaf, supporting the idea that CHD3 proteins and PcG proteins antagonistically determine cell identity in plants. The direct targets of PKL in roots include the PcG genes SWINGER and EMBRYONIC FLOWER2 that encode subunits of Polycomb repressive complexes responsible for trimethylating histone H3 at lysine 27 (H3K27me3). Similar to mutants lacking PcG proteins, lack of PKL and PKR2 caused reduced H3K27me3 levels and, therefore, increased expression of a set of PcG protein target genes in roots. Thus, PKL and PKR2 are directly required for activation of PcG protein target genes and in roots are also indirectly required for repression of PcG protein target genes. Reduced PcG protein activity can lead to cell de-differentiation and callus-like tissue formation in pkl pkr2 mutants. Thus, in contrast to mammals, where PcG proteins are required to maintain pluripotency and to prevent cell differentiation, in plants PcG proteins are required to promote cell differentiation by suppressing embryonic development.

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Section: Discussionsupporting

confidence: 94%

CHD3 Proteins and Polycomb Group Proteins Antagonistically Determine Cell Identity in Arabidopsis

Aichinger¹,

Villar²,

et al. 2009

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“…One of the mechanisms by which PKL represses gene expression is by promoting H3K27me3 deposition [45, 46]. The level of H3K9me2 is tightly linked to non-CG DNA methylation [13].…”

Section: Resultsmentioning

confidence: 99%

The developmental regulator PKL is required to maintain correct DNA methylation patterns at RNA-directed DNA methylation loci

et al. 2017

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BackgroundThe chromodomain helicase DNA-binding family of ATP-dependent chromatin remodeling factors play essential roles during eukaryote growth and development. They are recruited by specific transcription factors and regulate the expression of developmentally important genes. Here, we describe an unexpected role in non-coding RNA-directed DNA methylation in Arabidopsis thaliana.ResultsThrough forward genetic screens we identified PKL, a gene required for developmental regulation in plants, as a factor promoting transcriptional silencing at the transgenic RD29A promoter. Mutation of PKL results in DNA methylation changes at more than half of the loci that are targeted by RNA-directed DNA methylation (RdDM). A small number of transposable elements and genes had reduced DNA methylation correlated with derepression in the pkl mutant, though for the majority, decreases in DNA methylation are not sufficient to cause release of silencing. The changes in DNA methylation in the pkl mutant are positively correlated with changes in 24-nt siRNA levels. In addition, PKL is required for the accumulation of Pol V-dependent transcripts and for the positioning of Pol V-stabilized nucleosomes at several tested loci, indicating that RNA polymerase V-related functions are impaired in the pkl mutant.Conclusions PKL is required for transcriptional silencing and has significant effects on RdDM in plants. The changes in DNA methylation in the pkl mutant are correlated with changes in the non-coding RNAs produced by Pol IV and Pol V. We propose that at RdDM target regions, PKL may be required to create a chromatin environment that influences non-coding RNA production, DNA methylation, and transcriptional silencing.Electronic supplementary materialThe online version of this article (doi:10.1186/s13059-017-1226-y) contains supplementary material, which is available to authorized users.

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“…The pkl mutant seedlings retain embryonic traits after germination and produce somatic embryos from a number of seedling tissues, coinciding with de‐repression of the LEC genes (Henderson et al., 2004; Ogas, Kaufmann, Henderson, & Somerville, 1999). CHD3 proteins are associated with histone deacetylases in animals (Torchy, Hamiche, & Klaholz, 2015), but loss of PKL in plants was found to affect global H3K27me3 levels, also at the LEC1 and LEC2 loci, rather than acetylation levels (Zhang et al., 2008). However, HDAC activity has also been shown to be required for certain pkl phenotypes in plants (Fukaki, Taniguchi, & Tasaka, 2006), and TSA treatment could to a certain extent mimic pkl phenotypes in arabidopsis calli (Furuta et al., 2011), suggesting that PKL may function by guiding both H3K27me3 and histone deacetylation.…”

Section: The Role Of Chromatin Modifications In Somatic Embryogenesismentioning

confidence: 99%

A transcriptional view on somatic embryogenesis

2017

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Somatic embryogenesis is a form of induced plant cell totipotency where embryos develop from somatic or vegetative cells in the absence of fertilization. Somatic embryogenesis can be induced in vitro by exposing explants to stress or growth regulator treatments. Molecular genetics studies have also shown that ectopic expression of specific embryo‐ and meristem‐expressed transcription factors or loss of certain chromatin‐modifying proteins induces spontaneous somatic embryogenesis. We begin this review with a general description of the major developmental events that define plant somatic embryogenesis and then focus on the transcriptional regulation of this process in the model plant Arabidopsis thaliana (arabidopsis). We describe the different somatic embryogenesis systems developed for arabidopsis and discuss the roles of transcription factors and chromatin modifications in this process. We describe how these somatic embryogenesis factors are interconnected and how their pathways converge at the level of hormones. Furthermore, the similarities between the developmental pathways in hormone‐ and transcription‐factor‐induced tissue culture systems are reviewed in the light of our recent findings on the somatic embryo‐inducing transcription factor BABY BOOM.

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The CHD3 Remodeler PICKLE Promotes Trimethylation of Histone H3 Lysine 27

Cited by 131 publications

References 62 publications

CHD3 Proteins and Polycomb Group Proteins Antagonistically Determine Cell Identity in Arabidopsis

CHD3 Proteins and Polycomb Group Proteins Antagonistically Determine Cell Identity in Arabidopsis

The developmental regulator PKL is required to maintain correct DNA methylation patterns at RNA-directed DNA methylation loci

A transcriptional view on somatic embryogenesis

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