论文信息 - m6A RNA methylation regulates the UV-induced DNA damage response - 字舞流文

m6A RNA methylation regulates the UV-induced DNA damage response

Cell proliferation and survival require the faithful maintenance and propagation of genetic information, which are threatened by the ubiquitous sources of DNA damage present intracellularly and in the external environment. A system of DNA repair, called the DNA damage response, detects and repairs damaged DNA and prevents cell division until the repair is complete. Here we report that methylation at the 6 position of adenosine (m6A) in RNA is rapidly (within 2 min) and transiently induced at DNA damage sites in response to ultraviolet irradiation. This modification occurs on numerous poly(A)+ transcripts and is regulated by the methyltransferase METTL3 (methyltransferase-like 3) and the demethylase FTO (fat mass and obesity-associated protein). In the absence of METTL3 catalytic activity, cells showed delayed repair of ultraviolet-induced cyclobutane pyrimidine adducts and elevated sensitivity to ultraviolet, demonstrating the importance of m6A in the ultraviolet-responsive DNA damage response. Multiple DNA polymerases are involved in the ultraviolet response, some of which resynthesize DNA after the lesion has been excised by the nucleotide excision repair pathway, while others participate in trans-lesion synthesis to allow replication past damaged lesions in S phase. DNA polymerase κ (Pol κ), which has been implicated in both nucleotide excision repair and trans-lesion synthesis, required the catalytic activity of METTL3 for immediate localization to ultraviolet-induced DNA damage sites. Importantly, Pol κ overexpression qualitatively suppressed the cyclobutane pyrimidine removal defect associated with METTL3 loss. Thus, we have uncovered a novel function for RNA m6A modification in the ultraviolet-induced DNA damage response, and our findings collectively support a model in which m6A RNA serves as a beacon for the selective, rapid recruitment of Pol κ to damage sites to facilitate repair and cell survival.

Yang Shi | Chih-Hung Hsu | Chuan He | Zhike Lu | Chuan He | Yang Shi | A. Jambhekar | Chih-Hung Hsu | Sigrid Nachtergaele | L. Zou | P. Hsu | Hao Chen | Chuanyun Xu | Hao Chen | Zhike Lu | Sigrid Nachtergaele | Jian Ouyang | Ashwini Jambhekar | Yang Xiang | Benoit Laurent | Wanqiang Sheng | Chuanyun Xu | Hao Chen | Siqing Wang | Dominic Ling | Pang-Hung Hsu | Lee Zou | B. Laurent | Yang Xiang | Wanqiang Sheng | Siqing Wang | Dominic Ling | Jian Ouyang | Ouyang Jian | L. Zou | S. Nachtergaele | Benoit Laurent | Chih-Hung Hsu | Zhike Lu | Chuanyun Xu | Ouyang Jian | Pang-Hung Hsu | Lee Zou | Chuan He | Yang Shi

[1] Arne Klungland,et al. ALKBH5 is a mammalian RNA demethylase that impacts RNA metabolism and mouse fertility. , 2013, Molecular cell.

[2] D. Mitchell. THE RELATIVE CYTOTOXICITY OF(6–4) PHOTOPRODUCTS AND CYCLOBUTANE DIMERS IN MAMMALIAN CELLS * , 1988, Photochemistry and photobiology.

[3] A. Lehmann,et al. The Y-family DNA polymerase kappa (pol kappa) functions in mammalian nucleotide-excision repair. , 2006, Nature cell biology.

[4] Osamu Ogawa,et al. Involvement of Vertebrate Polκ in Rad18-independent Postreplication Repair of UV Damage* 210 , 2002, The Journal of Biological Chemistry.

[5] Cole Trapnell,et al. Transcript assembly and quantification by RNA-Seq reveals unannotated transcripts and isoform switching during cell differentiation. , 2010, Nature biotechnology.

[6] J. Svejstrup. The interface between transcription and mechanisms maintaining genome integrity. , 2010, Trends in biochemical sciences.

[7] F. Rottman,et al. Purification and cDNA cloning of the AdoMet-binding subunit of the human mRNA (N6-adenosine)-methyltransferase. , 1997, RNA.

[8] Atsushi Miyawaki,et al. Visualizing Spatiotemporal Dynamics of Multicellular Cell-Cycle Progression , 2008, Cell.

[9] Olivier Elemento,et al. 5′ UTR m6A Promotes Cap-Independent Translation , 2015, Cell.

[10] L. Aravind,et al. DNA Methylation on N6-Adenine in C. elegans , 2015, Cell.

[11] T. Ried,et al. H2AX Haploinsufficiency Modifies Genomic Stability and Tumor Susceptibility , 2003, Cell.

[12] Miao Yu,et al. A METTL3-METTL14 complex mediates mammalian nuclear RNA N6-adenosine methylation , 2013, Nature chemical biology.

[13] Yang Wang,et al. N6-methyladenosine modification destabilizes developmental regulators in embryonic stem cells , 2014, Nature Cell Biology.

[14] Chuan He,et al. N 6 -methyladenosine Modulates Messenger RNA Translation Efficiency , 2015, Cell.

[15] M. Liszewski,et al. Characterization of antibodies specific for N6-methyladenosine and for 7-methylguanosine. , 1977, Biochemistry.

[16] S. Elledge,et al. The DNA damage response: making it safe to play with knives. , 2010, Molecular cell.

[17] Qiang Wang,et al. Structural basis of N6-adenosine methylation by the METTL3–METTL14 complex , 2016, Nature.

[18] A. Lehmann,et al. The Y-family DNA polymerase κ (pol κ) functions in mammalian nucleotide-excision repair , 2006, Nature Cell Biology.

[19] L. Prakash,et al. Highly error-free role of DNA polymerase η in the replicative bypass of UV-induced pyrimidine dimers in mouse and human cells , 2009, Proceedings of the National Academy of Sciences.

[20] M. Yamaizumi,et al. Rad18 Regulates DNA Polymerase κ and Is Required for Recovery from S-Phase Checkpoint-Mediated Arrest , 2006, Molecular and Cellular Biology.

[21] Chengqi Yi,et al. N6-Methyladenosine in Nuclear RNA is a Major Substrate of the Obesity-Associated FTO , 2011, Nature chemical biology.

[22] Samir Adhikari,et al. Mammalian WTAP is a regulatory subunit of the RNA N6-methyladenosine methyltransferase , 2014, Cell Research.

[23] Gideon Rechavi,et al. Transcriptome-wide mapping of N6-methyladenosine by m6A-seq based on immunocapturing and massively parallel sequencing , 2013, Nature Protocols.

[24] Bing Ren,et al. N6-methyladenosine-dependent regulation of messenger RNA stability , 2013 .

[25] Erez Y. Levanon,et al. m6A mRNA methylation facilitates resolution of naïve pluripotency toward differentiation , 2015, Science.

[26] Mary Ellen Wiltrout,et al. Eukaryotic Translesion Polymerases and Their Roles and Regulation in DNA Damage Tolerance , 2009, Microbiology and Molecular Biology Reviews.

[27] S. Tavazoie,et al. N6-methyladenosine marks primary microRNAs for processing , 2015, Nature.

[28] Shu-Bing Qian,et al. Dynamic m6A mRNA methylation directs translational control of heat shock response , 2015, Nature.

[29] M. Kupiec,et al. Topology of the human and mouse m6A RNA methylomes revealed by m6A-seq , 2012, Nature.

[30] S. Elledge,et al. A chromatin localization screen reveals poly (ADP ribose)-regulated recruitment of the repressive polycomb and NuRD complexes to sites of DNA damage , 2010, Proceedings of the National Academy of Sciences.

[31] Samie R. Jaffrey,et al. m6A RNA methylation promotes XIST-mediated transcriptional repression , 2016, Nature.

[32] Joseph L DeRisi,et al. Unbiased selection of localization elements reveals cis-acting determinants of mRNA bud localization in Saccharomyces cerevisiae. , 2005, Proceedings of the National Academy of Sciences of the United States of America.

[33] Saeed Tavazoie,et al. HNRNPA2B1 Is a Mediator of m6A-Dependent Nuclear RNA Processing Events , 2015, Cell.

[34] P. Hanawalt,et al. Transcription-coupled DNA repair: two decades of progress and surprises , 2008, Nature Reviews Molecular Cell Biology.

[35] Y. Miki,et al. Three DNA polymerases, recruited by different mechanisms, carry out NER repair synthesis in human cells. , 2010, Molecular cell.