The histone variant H2A.W and linker histone H1 co-regulate heterochromatin accessibility and DNA methylation

Bourguet, Pierre; Picard, Colette L.; Yelagandula, Ramesh; Pélissier, Thierry; Lorković, Zdravko J.; Feng, Suhua; Pouch-Pélissier, Marie-Noëlle; Schmücker, Anna; Jacobsen, Steven E.; Berger, Frédéric; Mathieu, Olivier

doi:10.1101/2020.03.19.998609

Cited by 4 publications

(6 citation statements)

References 65 publications

(144 reference statements)

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“…4K) (Mathieu et al, 2003;Soppe et al, 2002) and CMT3 prefers features associated with stable (Figs . 4E,F,S4G) (Bourguet et al, 2021;Osakabe et al, 2018;Yelagandula et al, 2014) over unstable nucleosomes such as H2A.Z with active marks (Figs. 4H,I,S4H).…”

Section: Discussionmentioning

confidence: 91%

“…Indeed, CHG hypermethylation across the four groups was positively correlated with levels of the stable histone variants H2A, H2A.X and most notably H2A.W that was recently shown to be required for CHG methylation (Figs . 4E,F,S4G) (Bourguet et al, 2021;Yelagandula et al, 2014). CMT3-induced CHG hypermethylation was also tightly associated with transcriptionally repressive H3K9me2 marks, which are required for interdependent feedback loops with CMT3 (Fig.…”

Section: Chromatin Features Associated With Cmt3induced Gene Methylationmentioning

confidence: 98%

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Repression of CHROMOMETHYLASE 3 Prevents Epigenetic Collateral Damage in Arabidopsis

Papareddy

Páldi

Smolka

et al. 2021

Preprint

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DNA methylation has evolved to silence mutagenic transposable elements (TEs) while typically avoiding the targeting of endogenous genes. Mechanisms that prevent DNA methyltransferases from ectopically methylating genes are expected to be of prime importance during periods of dynamic cell cycle activities including plant embryogenesis. However, virtually nothing is known regarding how DNA methyltransferase activities are precisely regulated during embryogenesis to prevent the induction of potentially deleterious and mitotically stable genic epimutations. Here, we report that microRNA-mediated repression of CHROMOMETHYLASE 3 (CMT3) and the chromatin features that CMT3 prefers help prevent ectopic methylation of thousands of genes during embryogenesis that can persist for weeks afterwards. Moreover, CMT3-induced ectopic methylation of genes undergoing transcriptional activation can reduce their corresponding transcript levels. Therefore, the repression of CMT3 prevents epigenetic collateral damage on endogenous genes. We also provide a model that may help reconcile conflicting viewpoints regarding the functions of gene-body methylation that occurs in nearly all flowering plants.

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Section: Discussionmentioning

confidence: 91%

Section: Chromatin Features Associated With Cmt3induced Gene Methylationmentioning

confidence: 98%

Repression of CHROMOMETHYLASE 3 Prevents Epigenetic Collateral Damage in Arabidopsis

Papareddy

Páldi

Smolka

et al. 2021

Preprint

View full text Add to dashboard Cite

show abstract

“…clusters 2-4) (Figure 4-figure supplement 1I,J), we hypothesized that histone variants conferring differential nucleosome stabilities and chromatin accessibility may influence ectopic CMT3-induced hypermethylation (Osakabe et al, 2018). Indeed, CHG hypermethylation across the four groups was positively correlated with levels of the stable histone variants H2A, H2A.X and most notably H2A.W that was recently shown to be required for CHG methylation (Figure 4E,F, Figure 4-figure supplement 1K) (Bourguet et al, 2021;Yelagandula et al, 2014). CMT3-induced CHG hypermethylation was also tightly associated with transcriptionally repressive H3K9me2 marks, which are required for interdependent feedback loops with CMT3 (Figure 4G).…”

Section: Chromatin Features Associated With Cmt3-induced Gene Methylationmentioning

confidence: 88%

Repression of CHROMOMETHYLASE 3 prevents epigenetic collateral damage in Arabidopsis

Papareddy

Páldi

Smolka

et al. 2021

eLife

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DNA methylation has evolved to silence mutagenic transposable elements (TEs) while typically avoiding the targeting of endogenous genes. Mechanisms that prevent DNA methyltransferases from ectopically methylating genes are expected to be of prime importance during periods of dynamic cell cycle activities including plant embryogenesis. However, virtually nothing is known regarding how DNA methyltransferase activities are precisely regulated during embryogenesis to prevent the induction of potentially deleterious and mitotically stable genic epimutations. Here, we report that microRNA-mediated repression of CHROMOMETHYLASE 3 (CMT3) and the chromatin features that CMT3 prefers help prevent ectopic methylation of thousands of genes during embryogenesis that can persist for weeks afterwards. Our results are also consistent with CMT3-induced ectopic methylation of promoters or bodies of genes undergoing transcriptional activation reducing their expression. Therefore, the repression of CMT3 prevents epigenetic collateral damage on endogenous genes. We also provide a model that may help reconcile conflicting viewpoints regarding the functions of gene-body methylation that occurs in nearly all flowering plants.

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“…Actually, a large genomic rearrangement in one of the T-DNA insertion mutant allele hindered proper functional analysis of H2A.W: the initially reported severe developmental and heterochromatin defects, rather than being caused by the loss of H2A.W function, were due to a duplication of the CMT3 locus. This was revealed by a newly constructed CRISPR-Cas9-induced null h2a.w triple mutant, which displayed no visible developmental phenotypes and had only minor effects on gene expression [ 51 ]. The CRISPR-Cas9 editing tool thus brings new perspectives, notably avoiding T-DNA-induced wide genomic rearrangements with unexpected effects on the epigenome.…”

Section: Direct Gene Manipulation For Genome-wide Chromatin Modulamentioning

confidence: 99%

“…A report describes the editing of histone H2A variants (H2AX and macroH2A, involved in DNA Damage Response) using CRISPR-Cas9 in human cells [ 52 ]. In plants, the above mentioned CRISPR-Cas9-induced new null h2a.w triple mutant (part 4.1) showed that H2A.W fine-tunes the accessibility of heterochromatin by preventing deposition of the linker Histone H1, thereby facilitating access to non-CG DNA methylation factors [ 51 ].…”

Section: Direct Gene Manipulation For Genome-wide Chromatin Modulamentioning

confidence: 99%

Chromatin Manipulation and Editing: Challenges, New Technologies and Their Use in Plants

Fal

Tomkova

Vachon

et al. 2021

IJMS

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An ongoing challenge in functional epigenomics is to develop tools for precise manipulation of epigenetic marks. These tools would allow moving from correlation-based to causal-based findings, a necessary step to reach conclusions on mechanistic principles. In this review, we describe and discuss the advantages and limits of tools and technologies developed to impact epigenetic marks, and which could be employed to study their direct effect on nuclear and chromatin structure, on transcription, and their further genuine role in plant cell fate and development. On one hand, epigenome-wide approaches include drug inhibitors for chromatin modifiers or readers, nanobodies against histone marks or lines expressing modified histones or mutant chromatin effectors. On the other hand, locus-specific approaches consist in targeting precise regions on the chromatin, with engineered proteins able to modify epigenetic marks. Early systems use effectors in fusion with protein domains that recognize a specific DNA sequence (Zinc Finger or TALEs), while the more recent dCas9 approach operates through RNA-DNA interaction, thereby providing more flexibility and modularity for tool designs. Current developments of “second generation”, chimeric dCas9 systems, aiming at better targeting efficiency and modifier capacity have recently been tested in plants and provided promising results. Finally, recent proof-of-concept studies forecast even finer tools, such as inducible/switchable systems, that will allow temporal analyses of the molecular events that follow a change in a specific chromatin mark.

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The histone variant H2A.W and linker histone H1 co-regulate heterochromatin accessibility and DNA methylation

Cited by 4 publications

References 65 publications

Repression of CHROMOMETHYLASE 3 Prevents Epigenetic Collateral Damage in Arabidopsis

Repression of CHROMOMETHYLASE 3 Prevents Epigenetic Collateral Damage in Arabidopsis

Repression of CHROMOMETHYLASE 3 prevents epigenetic collateral damage in Arabidopsis

Chromatin Manipulation and Editing: Challenges, New Technologies and Their Use in Plants

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