Histone H3 trimethylation at lysine 36 guides m6A RNA modification co-transcriptionally.

Huang, Weng, Zhou, Wu, Zhao et al.
Nature 2019
Open on PubMed

DNA and histone modifications have notable effects on gene expression1. Being the most prevalent internal modification in mRNA, the N6-methyladenosine (m6A) mRNA modification is as an important post-transcriptional mechanism of gene regulation2-4 and has crucial roles in various normal and pathological processes5-12. However, it is unclear how m6A is specifically and dynamically deposited in the transcriptome. Here we report that histone H3 trimethylation at Lys36 (H3K36me3), a marker for transcription elongation, guides m6A deposition globally. We show that m6A modifications are enriched in the vicinity of H3K36me3 peaks, and are reduced globally when cellular H3K36me3 is depleted. Mechanistically, H3K36me3 is recognized and bound directly by METTL14, a crucial component of the m6A methyltransferase complex (MTC), which in turn facilitates the binding of the m6A MTC to adjacent RNA polymerase II, thereby delivering the m6A MTC to actively transcribed nascent RNAs to deposit m6A co-transcriptionally. In mouse embryonic stem cells, phenocopying METTL14 knockdown, H3K36me3 depletion also markedly reduces m6A abundance transcriptome-wide and in pluripotency transcripts, resulting in increased cell stemness. Collectively, our studies reveal the important roles of H3K36me3 and METTL14 in determining specific and dynamic deposition of m6A in mRNA, and uncover another layer of gene expression regulation that involves crosstalk between histone modification and RNA methylation.

14 Figures Extracted
Extended Data Figure 1. Pmc_Xml
Overlapping of H3K36me3 with m 6 (a) Overlaps of m 6 6 6 GSE37003 6 6 6 r P
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Extended Data Figure 2. Pmc_Xml
Cellular m 6 (a) Western blot showing knockdown efficiency of SETD2 and decrease of H3K36me3 in HepG2 and Hela cells by shSETD2#1. GAPDH and H3 serve as loading controls. (b) LC-MS/MS quantification o...
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Extended Data Figure 3. Pmc_Xml
Reprogramming of H3K36me3 and m 6 (a) Histogram showing H3K36me3 peak numbers in HepG2 cells with (shSETD2#1) or without (shCtrl) SETD2 knockdown. (b) Cumulative curves and box plot showing reduction ...
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Extended Data Figure 4. Pmc_Xml
Genome-/Transcriptome-wide and locus-specific co-regulation of H3K36me3 and m 6 (a) Circos plot showing global distribution of H3K36me3 and m 6 6 6 6 6 6 6 6 6 6 6 6 6 6 P P P
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Extended Data Figure 5. Pmc_Xml
Locus-specific regulation of m 6 (a, b) Schematic showing the epigenetic editing of H3K36me3 by dCas9-KDM4A on MYC-CRD (a) or by dCas-SETD2 on GNG4 (b). (c) Distribution of H3K36me3 and m 6 GNG4 6 6 P
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Extended Data Figure 6. Pmc_Xml
Impact of SETD2 knockdown on gene expression, mRNA stability and translation. (a) Distribution of H3K36me3 and m 6 MYC 2 P 2 P P 1/2 MYC 2 P 2 P r P
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Extended Data Figure 7. Pmc_Xml
Mechanism of H3K36me3-dependent m 6 (a) Binding of METTL3 (MTL3, upper panel) and METTL14 (MTL14, lower panel) to target mRNAs was determined by CLIP-qPCR assays. (b) qPCR data showing that knockdown ...
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Extended Data Figure 8. Pmc_Xml
METTL14 binds to H3K36me3 in vitro in vivo (a) Schematic of the indirect or direct models of H3K36me3 recruiting MTC. “Adaptor” model (left) refers to indirect interaction of m 6 6 6 in vitro 6 6 6 P...
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Extended Data Figure 9. Pmc_Xml
Silencing of SETD2 demethylates H3K36me3 and m 6 in vitro (a) qPCR showing remarkable downregulation of SETD2, but not m 6 in vitro th th th th P 6 6 6 th th th th P P 6 6 58 P P P
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Extended Data Figure 10. Pmc_Xml
Impact of SETD2 and METTL14 in mESCs differentiation. (a and b) qPCR detecting the expression of SETD2 METTL14 in vitro SETD2 METTL14 in vitro P P P
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Figure 1. Pmc_Xml
H3K36me3 histone modification affects de novo 6 (a) LC-MS/MS quantification of m 6 6 6 6 6 6 6 6 6 MYC 6 6 P P P
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Figure 2. Pmc_Xml
Transcriptome-wide cooperation of H3K36me3 and MTC in m 6 (a) Venn diagram of significantly hypomethylated peaks in HepG2 cells upon knockdown of SETD2 (shSETD2#1) or individual m 6 6 6 P 6 6 r P
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Figure 3. Pmc_Xml
H3K36me3 is recognized by METTL14 and guides m 6 (a) Co-immunoprecipitation and western blot in Hela cells with forced expression of HA-tagged m 6 6 6
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Figure 4. Pmc_Xml
Loss of H3K36me3 reduces m 6 in vitro (a) Western blot showing increase of pluripotency factors in mESCs with Dox-induced SETD2 knockdown. (b) Distribution of genes with more than 1.5 fold changes ( P...
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