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首页> 外文期刊>Radiation oncology >Tumor treating fields (TTFields) delay DNA damage repair following radiation treatment of glioma cells
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Tumor treating fields (TTFields) delay DNA damage repair following radiation treatment of glioma cells

机译:胶质瘤细胞放射治疗后的肿瘤治疗场(TTFields)延迟了DNA损伤修复

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摘要

Tumor Treating Fields (TTFields) are an anti-neoplastic treatment modality delivered via application of alternating electric fields using insulated transducer arrays placed directly on the skin in the region surrounding the tumor. A Phase 3 clinical trial has demonstrated the effectiveness of continuous TTFields application in patients with glioblastoma during maintenance treatment with Temozolomide. The goal of this study was to evaluate the efficacy of combining TTFields with radiation treatment (RT) in glioma cells. We also examined the effect of TTFields transducer arrays on RT distribution in a phantom model and the impact on rat skin toxicity. The efficacy of TTFields application after induction of DNA damage by RT or bleomycin was tested in U-118 MG and LN-18 glioma cells. The alkaline comet assay was used to measure repair of DNA lesions. Repair of DNA double strand breaks (DSBs) were assessed by analyzing γH2AX or Rad51 foci. DNA damage and repair signaled by the activation pattern of phospho-ATM (pS1981) and phospho-DNA-PKcs (pS2056) was evaluated by immunoblotting. The absorption of the RT energy by transducer arrays was measured by applying RT through arrays placed on a solid-state phantom. Skin toxicities were tested in rats irradiated daily through the arrays with 2Gy (total dose of 20Gy). TTFields synergistically enhanced the efficacy of RT in glioma cells. Application of TTFields to irradiated cells impaired repair of irradiation- or chemically-induced DNA damage, possibly by blocking homologous recombination repair. Transducer arrays presence caused a minor reduction in RT intensity at 20?mm and 60?mm below the arrays, but led to a significant increase in RT dosage at the phantom surface jeopardizing the “skin sparing effect”. Nevertheless, transducer arrays placed on the rat skin during RT did not lead to additional skin reactions. Administration of TTFields after RT increases glioma cells treatment efficacy possibly by inhibition of DNA damage repair. These preclinical results support the application of TTFields therapy immediately after RT as a viable regimen to enhance RT outcome. Phantom measurements and animal models imply that it may be possible to leave the transducer arrays in place during RT without increasing skin toxicities.
机译:肿瘤治疗场(TTFields)是一种抗肿瘤治疗方式,通过使用绝缘换能器阵列直接施加在肿瘤周围区域的皮肤上,通过施加交变电场来提供。一项3期临床试验表明,在替莫唑胺维持治疗期间,连续应用TTFields对胶质母细胞瘤患者有效。这项研究的目的是评估胶质瘤细胞中结合TTFields与放射治疗(RT)的疗效。我们还检查了幻影模型中TTFields传感器阵列对RT分布的影响以及对大鼠皮肤毒性的影响。在U-118 MG和LN-18胶质瘤细胞中测试了RT或博来霉素诱导的DNA损伤后TTFields应用的功效。碱性彗星试验用于测量DNA损伤的修复。通过分析γH2AX或Rad51病灶评估DNA双链断裂(DSB)的修复。通过免疫印迹评估了磷酸ATM(pS1981)和磷酸DNA-PKcs(pS2056)激活模式所指示的DNA损伤和修复。换能器阵列对RT能量的吸收是通过对放置在固态体模上的阵列施加RT来测量的。在每天用2Gy(总剂量20Gy)通过阵列照射的大鼠中测试了皮肤毒性。 TTFields协同增强了RT在神经胶质瘤细胞中的功效。 TTFields在辐照细胞上的应用可能通过阻断同源重组修复而损害了辐照或化学诱导的DNA损伤的修复。换能器阵列的存在导致阵列下方的20?mm和60?mm处的RT强度略有降低,但导致幻影表面的RT剂量显着增加,损害了“节省皮肤的作用”。然而,在RT期间放置在大鼠皮肤上的换能器阵列并不会导致其他皮肤反应。 RT后给予TTFields可能通过抑制DNA损伤修复来提高神经胶质瘤细胞的治疗功效。这些临床前结果支持在RT后立即应用TTFields治疗,作为增强RT结果的可行方案。幻像测量和动物模型暗示在RT期间有可能将换能器阵列留在原地而不会增加皮肤毒性。

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