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The histone mark H3K36me2 recruits DNMT3A and shapes the intergenic DNA methylation landscape

Author

Listed:
  • Daniel N. Weinberg

    (The Rockefeller University)

  • Simon Papillon-Cavanagh

    (McGill University)

  • Haifen Chen

    (McGill University)

  • Yuan Yue

    (Tsinghua University)

  • Xiao Chen

    (Columbia University Irving Medical Center
    Columbia University Irving Medical Center)

  • Kartik N. Rajagopalan

    (Columbia University Irving Medical Center)

  • Cynthia Horth

    (McGill University)

  • John T. McGuire

    (Columbia University Irving Medical Center
    Columbia University Irving Medical Center)

  • Xinjing Xu

    (Columbia University Irving Medical Center
    Columbia University Irving Medical Center)

  • Hamid Nikbakht

    (McGill University)

  • Agata E. Lemiesz

    (The Rockefeller University)

  • Dylan M. Marchione

    (University of Pennsylvania
    University of Pennsylvania)

  • Matthew R. Marunde

    (EpiCypher Inc)

  • Matthew J. Meiners

    (EpiCypher Inc)

  • Marcus A. Cheek

    (EpiCypher Inc)

  • Michael-Christopher Keogh

    (EpiCypher Inc)

  • Eric Bareke

    (McGill University)

  • Anissa Djedid

    (McGill University)

  • Ashot S. Harutyunyan

    (McGill University)

  • Nada Jabado

    (McGill University
    McGill University
    Research Institute of the McGill University Health Center)

  • Benjamin A. Garcia

    (University of Pennsylvania
    University of Pennsylvania)

  • Haitao Li

    (Tsinghua University)

  • C. David Allis

    (The Rockefeller University)

  • Jacek Majewski

    (McGill University)

  • Chao Lu

    (Columbia University Irving Medical Center
    Columbia University Irving Medical Center)

Abstract

Enzymes that catalyse CpG methylation in DNA, including the DNA methyltransferases 1 (DNMT1), 3A (DNMT3A) and 3B (DNMT3B), are indispensable for mammalian tissue development and homeostasis1–4. They are also implicated in human developmental disorders and cancers5–8, supporting the critical role of DNA methylation in the specification and maintenance of cell fate. Previous studies have suggested that post-translational modifications of histones are involved in specifying patterns of DNA methyltransferase localization and DNA methylation at promoters and actively transcribed gene bodies9–11. However, the mechanisms that control the establishment and maintenance of intergenic DNA methylation remain poorly understood. Tatton–Brown–Rahman syndrome (TBRS) is a childhood overgrowth disorder that is defined by germline mutations in DNMT3A. TBRS shares clinical features with Sotos syndrome (which is caused by haploinsufficiency of NSD1, a histone methyltransferase that catalyses the dimethylation of histone H3 at K36 (H3K36me2)8,12,13), which suggests that there is a mechanistic link between these two diseases. Here we report that NSD1-mediated H3K36me2 is required for the recruitment of DNMT3A and maintenance of DNA methylation at intergenic regions. Genome-wide analysis shows that the binding and activity of DNMT3A colocalize with H3K36me2 at non-coding regions of euchromatin. Genetic ablation of Nsd1 and its paralogue Nsd2 in mouse cells results in a redistribution of DNMT3A to H3K36me3-modified gene bodies and a reduction in the methylation of intergenic DNA. Blood samples from patients with Sotos syndrome and NSD1-mutant tumours also exhibit hypomethylation of intergenic DNA. The PWWP domain of DNMT3A shows dual recognition of H3K36me2 and H3K36me3 in vitro, with a higher binding affinity towards H3K36me2 that is abrogated by TBRS-derived missense mutations. Together, our study reveals a trans-chromatin regulatory pathway that connects aberrant intergenic CpG methylation to human neoplastic and developmental overgrowth.

Suggested Citation

  • Daniel N. Weinberg & Simon Papillon-Cavanagh & Haifen Chen & Yuan Yue & Xiao Chen & Kartik N. Rajagopalan & Cynthia Horth & John T. McGuire & Xinjing Xu & Hamid Nikbakht & Agata E. Lemiesz & Dylan M. , 2019. "The histone mark H3K36me2 recruits DNMT3A and shapes the intergenic DNA methylation landscape," Nature, Nature, vol. 573(7773), pages 281-286, September.
    • Handle: RePEc:nat:nature:v:573:y:2019:i:7773:d:10.1038_s41586-019-1534-3
    DOI: 10.1038/s41586-019-1534-3
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    Citations

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    Cited by:

    1. Naoki Kubo & Ryuji Uehara & Shuhei Uemura & Hiroaki Ohishi & Kenjiro Shirane & Hiroyuki Sasaki, 2024. "Combined and differential roles of ADD domains of DNMT3A and DNMT3L on DNA methylation landscapes in mouse germ cells," Nature Communications, Nature, vol. 15(1), pages 1-12, December.
    2. Yafei Jiang & Jinzeng Wang & Mengxiong Sun & Dongqing Zuo & Hongsheng Wang & Jiakang Shen & Wenyan Jiang & Haoran Mu & Xiaojun Ma & Fei Yin & Jun Lin & Chongren Wang & Shuting Yu & Lu Jiang & Gang Lv , 2022. "Multi-omics analysis identifies osteosarcoma subtypes with distinct prognosis indicating stratified treatment," Nature Communications, Nature, vol. 13(1), pages 1-17, December.
    3. Ko Sato & Amarjeet Kumar & Keisuke Hamada & Chikako Okada & Asako Oguni & Ayumi Machiyama & Shun Sakuraba & Tomohiro Nishizawa & Osamu Nureki & Hidetoshi Kono & Kazuhiro Ogata & Toru Sengoku, 2021. "Structural basis of the regulation of the normal and oncogenic methylation of nucleosomal histone H3 Lys36 by NSD2," Nature Communications, Nature, vol. 12(1), pages 1-10, December.
    4. Xiao Chen & Yinglu Li & Fang Zhu & Xinjing Xu & Brian Estrella & Manuel A. Pazos & John T. McGuire & Dimitris Karagiannis & Varun Sahu & Mustafo Mustafokulov & Claudio Scuoppo & Francisco J. Sánchez-R, 2023. "Context-defined cancer co-dependency mapping identifies a functional interplay between PRC2 and MLL-MEN1 complex in lymphoma," Nature Communications, Nature, vol. 14(1), pages 1-17, December.
    5. Seiichi Yano & Takashi Ishiuchi & Shusaku Abe & Satoshi H. Namekawa & Gang Huang & Yoshihiro Ogawa & Hiroyuki Sasaki, 2022. "Histone H3K36me2 and H3K36me3 form a chromatin platform essential for DNMT3A-dependent DNA methylation in mouse oocytes," Nature Communications, Nature, vol. 13(1), pages 1-12, December.
    6. Kentaro Mochizuki & Jafar Sharif & Kenjiro Shirane & Kousuke Uranishi & Aaron B. Bogutz & Sanne M. Janssen & Ayumu Suzuki & Akihiko Okuda & Haruhiko Koseki & Matthew C. Lorincz, 2021. "Repression of germline genes by PRC1.6 and SETDB1 in the early embryo precedes DNA methylation-mediated silencing," Nature Communications, Nature, vol. 12(1), pages 1-15, December.
    7. Jiuwei Lu & Yiran Guo & Jiekai Yin & Jianbin Chen & Yinsheng Wang & Gang Greg Wang & Jikui Song, 2024. "Structure-guided functional suppression of AML-associated DNMT3A hotspot mutations," Nature Communications, Nature, vol. 15(1), pages 1-16, December.

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