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首页> 外文期刊>International Journal of Radiation Oncology, Biology, Physics >Radiation-induced DNA damage and repair in lymphocytes from breast cancer patients and their correlation with acute skin reactions to radiotherapy.
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Radiation-induced DNA damage and repair in lymphocytes from breast cancer patients and their correlation with acute skin reactions to radiotherapy.

机译:辐射诱导的乳腺癌患者淋巴细胞的DNA损伤和修复及其与放射治疗的急性皮肤反应的相关性。

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摘要

Repair of radiation-induced DNA damage plays a critical role for both the susceptibility of patients to side effects after radiotherapy and their subsequent cancer risk. The study objective was to evaluate whether DNA repair data determined in vitro are correlated with the occurrence of acute side effects during radiotherapy.Breast cancer patients receiving radiation therapy after a breast-conserving surgery were recruited in a prospective epidemiologic study. As an indicator for clinical radiosensitivity, adverse reactions of the skin were recorded. Cryo-preserved lymphocytes from 113 study participants were gamma-irradiated with 5 Gy in vitro and analyzed using the alkaline comet assay. Reproducibility of the assay was determined by repeated analysis (n = 26) of cells from a healthy donor. A coefficient of variation of 0.3 was calculated.The various parameters determined to characterize the individual DNA repair capacity showed large differences between patients. Eleven patients were identified with considerably enhanced DNA damage induction, and 7 patients exhibited severely reduced DNA repair capacity after 15 and 30 min. Six patients were considered as clinically radiosensitive, indicated by moist desquamation of the skin after a total radiation dose of about 50 Gy.Using the alkaline comet assay as described here, breast cancer patients were identified showing abnormal cellular radiation effects, but this repair deficiency corresponded only at a very limited extent to the acute radiation sensitivity of the skin. Because impaired DNA repair could be involved in the development of late irradiation effects, individuals exhibiting severely reduced DNA repair capacity should be followed for the development of late clinical symptoms.
机译:放射线诱发的DNA损伤的修复对于放疗后的患者易感性及其随后的癌症风险起着至关重要的作用。本研究的目的是评估体外测定的DNA修复数据是否与放疗期间发生的急性副作用相关。在一项前瞻性流行病学研究中,招募了接受保乳手术后接受放射治疗的乳腺癌患者。作为临床放射敏感性的指标,记录了皮肤的不良反应。来自113位研究参与者的冷冻保存的淋巴细胞在体外用5 Gyγ射线照射,并使用碱性彗星试验进行了分析。通过对健康供体的细胞进行重复分析(n = 26)来确定测定的可重复性。计算出的变异系数为0.3。为表征个体DNA修复能力而确定的各种参数在患者之间存在很大差异。鉴定出11名患者的DNA损伤诱导明显增强,而7名患者在15和30分钟后表现出严重的DNA修复能力降低。总辐射剂量约50 Gy后皮肤湿润脱皮,表明有6名患者具有临床放射敏感性。使用此处所述的碱性彗星试验检测出乳腺癌患者显示出异常的细胞辐射效应,但这种修复缺陷对应仅在非常有限的程度上对皮肤的急性放射敏感性。由于受损的DNA修复可能与晚期放射效应的发展有关,因此对于晚期临床症状的发生,应该跟踪表现出严重降低的DNA修复能力的个体。

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