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m5C modification of mRNA serves a DNA damage code to promote homologous recombination

Author

Listed:
  • Hao Chen

    (University of Pittsburgh School of Medicine)

  • Haibo Yang

    (Harvard Medical School
    Harvard Medical School)

  • Xiaolan Zhu

    (Harvard Medical School)

  • Tribhuwan Yadav

    (Harvard Medical School)

  • Jian Ouyang

    (Harvard Medical School
    Harvard Medical School)

  • Samuel S. Truesdell

    (Harvard Medical School
    Harvard Medical School)

  • Jun Tan

    (Harvard Medical School
    Harvard Medical School)

  • Yumin Wang

    (University of Pittsburgh School of Medicine
    Harvard Medical School)

  • Meihan Duan

    (University of Pittsburgh School of Medicine)

  • Leizhen Wei

    (University of Pittsburgh School of Medicine)

  • Lee Zou

    (Harvard Medical School
    Harvard Medical School)

  • Arthur S. Levine

    (University of Pittsburgh School of Medicine)

  • Shobha Vasudevan

    (Harvard Medical School
    Harvard Medical School)

  • Li Lan

    (University of Pittsburgh School of Medicine
    Harvard Medical School
    Harvard Medical School)

Abstract

Recruitment of DNA repair proteins to DNA damage sites is a critical step for DNA repair. Post-translational modifications of proteins at DNA damage sites serve as DNA damage codes to recruit specific DNA repair factors. Here, we show that mRNA is locally modified by m5C at sites of DNA damage. The RNA methyltransferase TRDMT1 is recruited to DNA damage sites to promote m5C induction. Loss of TRDMT1 compromises homologous recombination (HR) and increases cellular sensitivity to DNA double-strand breaks (DSBs). In the absence of TRDMT1, RAD51 and RAD52 fail to localize to sites of reactive oxygen species (ROS)-induced DNA damage. In vitro, RAD52 displays an increased affinity for DNA:RNA hybrids containing m5C-modified RNA. Loss of TRDMT1 in cancer cells confers sensitivity to PARP inhibitors in vitro and in vivo. These results reveal an unexpected TRDMT1-m5C axis that promotes HR, suggesting that post-transcriptional modifications of RNA can also serve as DNA damage codes to regulate DNA repair.

Suggested Citation

  • Hao Chen & Haibo Yang & Xiaolan Zhu & Tribhuwan Yadav & Jian Ouyang & Samuel S. Truesdell & Jun Tan & Yumin Wang & Meihan Duan & Leizhen Wei & Lee Zou & Arthur S. Levine & Shobha Vasudevan & Li Lan, 2020. "m5C modification of mRNA serves a DNA damage code to promote homologous recombination," Nature Communications, Nature, vol. 11(1), pages 1-12, December.
    • Handle: RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-16722-7
    DOI: 10.1038/s41467-020-16722-7
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    Cited by:

    1. Ilaria Rosso & Corey Jones-Weinert & Francesca Rossiello & Matteo Cabrini & Silvia Brambillasca & Leonel Munoz-Sagredo & Zeno Lavagnino & Emanuele Martini & Enzo Tedone & Massimiliano Garre’ & Julio A, 2023. "Alternative lengthening of telomeres (ALT) cells viability is dependent on C-rich telomeric RNAs," Nature Communications, Nature, vol. 14(1), pages 1-16, December.
    2. Katja Hartstock & Nadine A. Kueck & Petr Spacek & Anna Ovcharenko & Sabine Hüwel & Nicolas V. Cornelissen & Amarnath Bollu & Christoph Dieterich & Andrea Rentmeister, 2023. "MePMe-seq: antibody-free simultaneous m6A and m5C mapping in mRNA by metabolic propargyl labeling and sequencing," Nature Communications, Nature, vol. 14(1), pages 1-19, December.

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