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首页> 外文期刊>International Journal of Radiation Oncology, Biology, Physics >Effects of motexafin gadolinium on DNA damage and X-ray-induced DNA damage repair, as assessed by the Comet assay.
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Effects of motexafin gadolinium on DNA damage and X-ray-induced DNA damage repair, as assessed by the Comet assay.

机译:彗星试验评估了莫特沙芬g对DNA损伤和X射线诱导的DNA损伤修复的影响。

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Purpose: To investigate the effects of motexafin gadolinium (MGd) on the levels of reactive oxygen species (ROS), glutathione (GSH), and DNA damage in EMT6 mouse mammary carcinoma cells. The ability of MGd to alter radiosensitivity and to inhibit DNA damage repair after X-ray irradiation was also evaluated. Methods and Materials: Reactive oxygen species and GSH levels were assessed by 2,7-dichlorofluorescein fluorescence flow cytometry and the Tietze method, respectively. Cellular radiosensitivity was assessed by clonogenic assays. Deoxyribonucleic acid damage and DNA damage repair were assessed in plateau-phase EMT6 cells by the Comet assay and clonogenic assays. Results: Cells treated with 100 mumol/L MGd plus equimolar ascorbic acid (AA) had significantly increased levels of ROS and a 58.9% +/- 3.4% decrease in GSH levels, relative to controls. Motexafin gadolinium plus AA treatment increased the hypoxic, but not the aerobic, radiosensitivity of EMT6 cells. There were increased levels of single-strand breaks in cells treated with 100 mumol/L MGd plus equimolar AA, as evidenced by changes in the alkaline tail moment (MGd + AA, 6 h: 14.7 +/- 1.8; control: 2.8 +/- 0.9). The level of single-strand breaks was dependent on the length of treatment. Motexafin gadolinium plus AA did not increase double-strand breaks. The repair of single-strand breaks at 2 h, but not at 4 h and 6 h, after irradiation was altered significantly in cells treated with MGd plus AA (MGd + AA, 2 h: 15.8 +/- 3.4; control: 5.8 +/- 0.6). Motexafin gadolinium did not alter the repair of double-strand breaks at any time after irradiation with 10 Gy. Conclusions: Motexafin gadolinium plus AA generated ROS, which in turn altered GSH homeostasis and induced DNA strand breaks. The MGd plus AA-mediated alteration of GSH levels increased the hypoxic, but not aerobic, radiosensitivity of EMT6 cells. Motexafin gadolinium altered the kinetics of single-strand break repair soon after irradiation but did not inhibit potentially lethal damage repair in EMT6 cells.
机译:目的:研究莫托沙芬g(MGd)对EMT6小鼠乳腺癌细胞中活性氧(ROS),谷胱甘肽(GSH)和DNA损伤水平的影响。还评估了MGd在X射线照射后改变放射敏感性和抑制DNA损伤修复的能力。方法和材料:分别通过2,7-二氯荧光素荧光流式细胞术和Tietze方法评估活性氧和GSH的含量。通过克隆形成测定法评估细胞的放射敏感性。通过彗星试验和克隆形成试验评估高原期EMT6细胞中的脱氧核糖核酸损伤和DNA损伤修复。结果:相对于对照,用100μmol/ L MGd加等摩尔抗坏血酸(AA)处理的细胞的ROS水平显着升高,GSH水平降低58.9%+/- 3.4%。 Motexafin plus加AA处理可增加EMT6细胞的低氧敏感性,但无氧敏感性。用100μmol/ L MGd和等摩尔AA处理的细胞中单链断裂的水平增加,这由碱性尾矩的变化所证实(MGd + AA,6小时:14.7 +/- 1.8;对照:2.8 + / -0.9)。单链断裂的水平取决于治疗时间。 Motexafin plus加AA不会增加双链断裂。在用MGd加AA(MGd + AA,2小时:15.8 +/- 3.4;对照:5.8 + /-0.6)。 Motexafin ado在10 Gy照射后的任何时间都不会改变双链断裂的修复。结论:Motexafin plus加AA生成ROS,从而改变GSH稳态并诱导DNA链断裂。 MGd加AA介导的GSH水平改变增加了EMT6细胞的低氧(但无氧)放射敏感性。 Motexafin ado在辐照后不久改变了单链断裂修复的动力学,但并未抑制EMT6细胞中潜在的致命损伤修复。

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