2022 Fiscal Year Final Research Report
The Mechanism of R-loop resolution in male germ cells and its effects on spermatogenesis and next generation.
| Project/Area Number |
21K20655
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| Research Category |
Grant-in-Aid for Research Activity Start-up
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| Allocation Type | Multi-year Fund |
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| Review Section |
0702:Biology at cellular to organismal levels, and related fields
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| Research Institution | Kyoto University |
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Principal Investigator |
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| Project Period (FY) |
2021-08-30 – 2023-03-31
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| Keywords | 精巣 / 精子幹細胞 / R-loop / DNA損傷 |
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| Outline of Final Research Achievements |
In this study, we established germline stem cells (GS cells) lacking Adar1, an R-loop resolution factor, and analyzed their DNA:RNA hybrid levels and gene expression. The DNA:RNA hybrid levels of whole genome in the cells were not affected by Adar1 knockout. On the other hand, the expression of p16INK4a, a senescence marker, was elevated in Adar1 knockout cells. This result suggests that Adar1 may contribute to cellular senescence in GS cells.
A screening for ADAR1-related factors in cultured cells identified ATM, TDP1, and XPF as candidate factors that function in regulation of R-loop. Further analysis is needed on the function of Adar1 in R-loop resolution by ATM, TDP1, and XPF in germ cells. Testis-specific Adar1-deficient mice have been generated and are currently being analyzed for effects on spermatogenesis and their offspring.
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| Free Research Field |
核酸発生生物学
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| Academic Significance and Societal Importance of the Research Achievements |
生殖細胞は次代に遺伝情報を伝達する細胞であり、その異常は次世代に受け継がれる。R-loop解消因子であるADAR1を欠損するGS細胞では細胞内全体のDNA:RNAハイブリッド量やインプリント遺伝子のDNAのメチルに変化は認められなかったが、ADAR1がTDP1などと協調して機能する可能性が示唆された。これらの成果はR-loop解消機構の理解に加え、カンプトテシンなどR-loopを誘導する抗がん剤に対する細胞の生存機構の理解にも繋がり、安全な薬剤使用に貢献できる。
ADAR1欠損GS細胞において老化マーカーであるp16の発現が上昇したことから、老化による男性不妊症の原因解明に繋がる可能性がある。
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