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Dive into the research topics where Mayumi Matsubara is active.

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Featured researches published by Mayumi Matsubara.


Journal of Biological Chemistry | 2009

Homologous recombination but not nucleotide excision repair plays a pivotal role in tolerance of DNA-protein cross-links in mammalian cells.

Toshiaki Nakano; Atsushi Katafuchi; Mayumi Matsubara; Hiroaki Terato; Tomohiro Tsuboi; Tasuku Masuda; Takahiro Tatsumoto; Seung Pil Pack; Keisuke Makino; Deborah L. Croteau; Bennett Van Houten; Kenta Iijima; Hiroshi Tauchi; Hiroshi Ide

DNA-protein cross-links (DPCs) are unique among DNA lesions in their unusually bulky nature. The steric hindrance imposed by cross-linked proteins (CLPs) will hamper DNA transactions, such as replication and transcription, posing an enormous threat to cells. In bacteria, DPCs with small CLPs are eliminated by nucleotide excision repair (NER), whereas oversized DPCs are processed exclusively by RecBCD-dependent homologous recombination (HR). Here we have assessed the roles of NER and HR for DPCs in mammalian cells. We show that the upper size limit of CLPs amenable to mammalian NER is relatively small (8–10 kDa) so that NER cannot participate in the repair of chromosomal DPCs in mammalian cells. Moreover, CLPs are not polyubiquitinated and hence are not subjected to proteasomal degradation prior to NER. In contrast, HR constitutes the major pathway in tolerance of DPCs as judged from cell survival and RAD51 and γ-H2AX nuclear foci formation. Induction of DPCs results in the accumulation of DNA double strand breaks in HR-deficient but not HR-proficient cells, suggesting that fork breakage at the DPC site initiates HR and reactivates the stalled fork. DPCs activate both ATR and ATM damage response pathways, but there is a time lag between two responses. These results highlight the differential involvement of NER in the repair of DPCs in bacterial and mammalian cells and demonstrate the versatile and conserved role of HR in tolerance of DPCs among species.


Biochemistry | 2003

Mammalian 5-Formyluracil−DNA Glycosylase. 2. Role of SMUG1 Uracil−DNA Glycosylase in Repair of 5-Formyluracil and Other Oxidized and Deaminated Base Lesions†

Aya Masaoka; Mayumi Matsubara; Rei Hasegawa; Tamon Tanaka; Satofumi Kurisu; Hiroaki Terato; Yoshihiko Ohyama; Naoko Karino; and Akira Matsuda; Hiroshi Ide


Molecular Cell | 2007

Nucleotide Excision Repair and Homologous Recombination Systems Commit Differentially to the Repair of DNA-Protein Crosslinks

Toshiaki Nakano; Soh Morishita; Atsushi Katafuchi; Mayumi Matsubara; Yusuke Horikawa; Hiroaki Terato; Amir M.H. Salem; Shunsuke Izumi; Seung Pil Pack; Keisuke Makino; Hiroshi Ide


Nucleic Acids Research | 2004

Mutational analysis of the damage-recognition and catalytic mechanism of human SMUG1 DNA glycosylase

Mayumi Matsubara; Tamon Tanaka; Hiroaki Terato; Eiji Ohmae; Shunsuke Izumi; Katsuo Katayanagi; Hiroshi Ide


Biochemistry | 2003

Mammalian 5-formyluracil-DNA glycosylase. 1. Identification and characterization of a novel activity that releases 5-formyluracil from DNA

Mayumi Matsubara; Aya Masaoka; Tamon Tanaka; Takayuki Miyano; Nagisa Kato; Hiroaki Terato; Yoshihiko Ohyama; Shigenori Iwai; Hiroshi Ide


DNA Repair | 2005

Roles of base excision repair enzymes Nth1p and Apn2p from Schizosaccharomyces pombe in processing alkylation and oxidative DNA damage

Takanori Sugimoto; Emi Igawa; Haruna Tanihigashi; Mayumi Matsubara; Hiroshi Ide; Shogo Ikeda


Nucleic acids research. Supplement (2001) | 2003

Identification and characterization of mammalian 5-formyluracil-DNA glycosylase

Mayumi Matsubara; Aya Masaoka; Tamon Tanaka; Hiroaki Terato; Yoshihiko Ohyama; Hiroshi Ide


Nucleic acids research. Supplement (2001) | 2003

Repair roles of hSMUG1 assessed by damage specificity and cellular activity

Aya Masaoka; Mayumi Matsubara; Tamon Tanaka; Hiroaki Terato; Yoshihiko Ohyama; Kihei Kubo; Hiroshi Ide


Nucleic acids symposium series (2004) | 2004

Damage specificity of human DNA glycosylases for oxidative pyrimidine lesions

Atsushi Katafuchi; Mayumi Matsubara; Hiroaki Terato; Shigenori Iwai; Fumio Hanaoka; Hiroshi Ide


Nucleic acids symposium series (2004) | 2005

Action mechanism of human SMUG1 uracil-DNA glycosylase

Mayumi Matsubara; Tamon Tanaka; Hiroaki Terato; Hiroshi Ide

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Aya Masaoka

National Institutes of Health

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Kihei Kubo

Osaka Prefecture University

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