Lauren de Wit, Maarten R Hamberg, Anne M Ross, Maaike Goris, Fia F Lie, Thomas Ruf, Sylvain Giroud, Robert H Henning, Roelof A Hut
{"title":"温度对冬眠期间 DNA 损伤的影响","authors":"Lauren de Wit, Maarten R Hamberg, Anne M Ross, Maaike Goris, Fia F Lie, Thomas Ruf, Sylvain Giroud, Robert H Henning, Roelof A Hut","doi":"10.1086/722904","DOIUrl":null,"url":null,"abstract":"<p><p>AbstractDuring multiday torpor, deep-hibernating mammals maintain a hypometabolic state where heart rate and ventilation are reduced to 2%-4% of euthermic rates. It is hypothesized that this ischemia-like condition may cause DNA damage through reactive oxygen species production. The reason for intermittent rewarming (arousal) during hibernation might be to repair the accumulated DNA damage. Because increasing ambient temperatures (<i>T</i><sub>a</sub>'s) shortens torpor bout duration, we hypothesize that hibernating at higher <i>T</i><sub>a</sub>'s will result in a faster accumulation of genomic DNA damage. To test this, we kept 39 male and female garden dormice at a <i>T</i><sub>a</sub> of either 5°C or 10°C and obtained tissue at 1, 4, and 8 d in torpor to assess DNA damage and recruitment of DNA repair markers in splenocytes. DNA damage in splenocytes measured by comet assay was significantly higher in almost all torpor groups than in summer euthermic groups. Damage accumulates in the first days of torpor at <math><mrow><msub><mrow><mi>T</mi></mrow><mrow><mi>a</mi></mrow></msub><mo>=</mo><msup><mrow><mn>5</mn></mrow><mrow><mo>°</mo></mrow></msup><mtext>C</mtext></mrow></math> (between days 1 and 4) but not at <math><mrow><msub><mrow><mi>T</mi></mrow><mrow><mi>a</mi></mrow></msub><mo>=</mo><msup><mrow><mn>10</mn></mrow><mrow><mo>°</mo></mrow></msup><mtext>C</mtext></mrow></math>. At the higher <i>T</i><sub>a</sub>, DNA damage is high at 24 h in torpor, indicating either a faster buildup of DNA damage at higher <i>T</i><sub>a</sub>'s or an incomplete repair during arousals in dormice. At 5°C, recruitment of the DNA repair protein 53BP1 paralleled the increase in DNA damage over time during torpor. In contrast, after 1 d in torpor at 10°C, DNA damage levels were high, but 53BP1 was not recruited to the nuclear DNA yet. The data suggest a potential mismatch in the DNA damage/repair dynamics during torpor at higher <i>T</i><sub>a</sub>'s.</p>","PeriodicalId":1,"journal":{"name":"Accounts of Chemical Research","volume":null,"pages":null},"PeriodicalIF":16.4000,"publicationDate":"2023-03-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Temperature Effects on DNA Damage during Hibernation.\",\"authors\":\"Lauren de Wit, Maarten R Hamberg, Anne M Ross, Maaike Goris, Fia F Lie, Thomas Ruf, Sylvain Giroud, Robert H Henning, Roelof A Hut\",\"doi\":\"10.1086/722904\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>AbstractDuring multiday torpor, deep-hibernating mammals maintain a hypometabolic state where heart rate and ventilation are reduced to 2%-4% of euthermic rates. It is hypothesized that this ischemia-like condition may cause DNA damage through reactive oxygen species production. The reason for intermittent rewarming (arousal) during hibernation might be to repair the accumulated DNA damage. Because increasing ambient temperatures (<i>T</i><sub>a</sub>'s) shortens torpor bout duration, we hypothesize that hibernating at higher <i>T</i><sub>a</sub>'s will result in a faster accumulation of genomic DNA damage. To test this, we kept 39 male and female garden dormice at a <i>T</i><sub>a</sub> of either 5°C or 10°C and obtained tissue at 1, 4, and 8 d in torpor to assess DNA damage and recruitment of DNA repair markers in splenocytes. DNA damage in splenocytes measured by comet assay was significantly higher in almost all torpor groups than in summer euthermic groups. Damage accumulates in the first days of torpor at <math><mrow><msub><mrow><mi>T</mi></mrow><mrow><mi>a</mi></mrow></msub><mo>=</mo><msup><mrow><mn>5</mn></mrow><mrow><mo>°</mo></mrow></msup><mtext>C</mtext></mrow></math> (between days 1 and 4) but not at <math><mrow><msub><mrow><mi>T</mi></mrow><mrow><mi>a</mi></mrow></msub><mo>=</mo><msup><mrow><mn>10</mn></mrow><mrow><mo>°</mo></mrow></msup><mtext>C</mtext></mrow></math>. At the higher <i>T</i><sub>a</sub>, DNA damage is high at 24 h in torpor, indicating either a faster buildup of DNA damage at higher <i>T</i><sub>a</sub>'s or an incomplete repair during arousals in dormice. At 5°C, recruitment of the DNA repair protein 53BP1 paralleled the increase in DNA damage over time during torpor. In contrast, after 1 d in torpor at 10°C, DNA damage levels were high, but 53BP1 was not recruited to the nuclear DNA yet. 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引用次数: 0
摘要
摘要在多日冬眠期间,深冬眠哺乳动物会保持低代谢状态,心率和通气量减少到呼气速率的 2%-4%。据推测,这种类似缺血的状态可能会通过活性氧的产生造成 DNA 损伤。冬眠期间间歇性复温(唤醒)的原因可能是为了修复累积的DNA损伤。由于环境温度(Ta's)的升高会缩短冬眠的持续时间,我们假设在较高的Ta's下冬眠会导致基因组DNA损伤的更快积累。为了验证这一假设,我们将39只雌雄花园睡鼠饲养在5°C或10°C的环境温度下,并在冬眠1、4和8天时采集它们的组织,以评估DNA损伤情况以及脾脏细胞中DNA修复标记物的招募情况。用彗星测定法测量,几乎所有冬眠组脾细胞中的DNA损伤都明显高于夏季信噪比组。在Ta=5°C的条件下,损伤在冬眠的最初几天(第1天和第4天之间)积累,而在Ta=10°C的条件下则没有积累。在较高的温度下,冬眠24小时后DNA损伤程度较高,这表明在较高的温度下DNA损伤积累较快,或者冬眠鼠在唤醒时修复不完全。在5°C条件下,DNA修复蛋白53BP1的招募与休眠期DNA损伤的增加同步。相反,在10°C条件下休眠1天后,DNA损伤水平很高,但53BP1尚未被招募到核DNA中。这些数据表明,在较高的温度下,冬眠过程中DNA损伤/修复动态可能存在不匹配。
Temperature Effects on DNA Damage during Hibernation.
AbstractDuring multiday torpor, deep-hibernating mammals maintain a hypometabolic state where heart rate and ventilation are reduced to 2%-4% of euthermic rates. It is hypothesized that this ischemia-like condition may cause DNA damage through reactive oxygen species production. The reason for intermittent rewarming (arousal) during hibernation might be to repair the accumulated DNA damage. Because increasing ambient temperatures (Ta's) shortens torpor bout duration, we hypothesize that hibernating at higher Ta's will result in a faster accumulation of genomic DNA damage. To test this, we kept 39 male and female garden dormice at a Ta of either 5°C or 10°C and obtained tissue at 1, 4, and 8 d in torpor to assess DNA damage and recruitment of DNA repair markers in splenocytes. DNA damage in splenocytes measured by comet assay was significantly higher in almost all torpor groups than in summer euthermic groups. Damage accumulates in the first days of torpor at (between days 1 and 4) but not at . At the higher Ta, DNA damage is high at 24 h in torpor, indicating either a faster buildup of DNA damage at higher Ta's or an incomplete repair during arousals in dormice. At 5°C, recruitment of the DNA repair protein 53BP1 paralleled the increase in DNA damage over time during torpor. In contrast, after 1 d in torpor at 10°C, DNA damage levels were high, but 53BP1 was not recruited to the nuclear DNA yet. The data suggest a potential mismatch in the DNA damage/repair dynamics during torpor at higher Ta's.
期刊介绍:
Accounts of Chemical Research presents short, concise and critical articles offering easy-to-read overviews of basic research and applications in all areas of chemistry and biochemistry. These short reviews focus on research from the author’s own laboratory and are designed to teach the reader about a research project. In addition, Accounts of Chemical Research publishes commentaries that give an informed opinion on a current research problem. Special Issues online are devoted to a single topic of unusual activity and significance.
Accounts of Chemical Research replaces the traditional article abstract with an article "Conspectus." These entries synopsize the research affording the reader a closer look at the content and significance of an article. Through this provision of a more detailed description of the article contents, the Conspectus enhances the article's discoverability by search engines and the exposure for the research.