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Higher Initial DNA Damage and Persistent Cell Cycle Arrest after Carbon Ion Irradiation Compared to X-irradiation in Prostate and Colon Cancer Cells

机译:与前列腺癌和结肠癌细胞的X射线照射相比碳离子照射后更高的初始DNA损伤和持久性细胞周期阻滞

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摘要

The use of charged-particle beams, such as carbon ions, is becoming a more and more attractive treatment option for cancer therapy. Given the precise absorbed dose-localization and an increased biological effectiveness, this form of therapy is much more advantageous compared to conventional radiotherapy, and is currently being used for treatment of specific cancer types. The high ballistic accuracy of particle beams deposits the maximal dose to the tumor, while damage to the surrounding healthy tissue is limited. In order to better understand the underlying mechanisms responsible for the increased biological effectiveness, we investigated the DNA damage and repair kinetics and cell cycle progression in two p53 mutant cell lines, more specifically a prostate (PC3) and colon (Caco-2) cancer cell line, after exposure to different radiation qualities. Cells were irradiated with various absorbed doses (0, 0.5, and 2 Gy) of accelerated 13C-ions at the Grand Accélérateur National d’Ions Lourds facility (Caen, France) or with X-rays (0, 0.1, 0.5, 1, 2, and 5 Gy). Microscopic analysis of DNA double-strand breaks showed dose-dependent increases in γ-H2AX foci numbers and foci occupancy after exposure to both types of irradiation, in both cell lines. However, 24 h after exposure, residual damage was more pronounced after lower doses of carbon ion irradiation compared to X-irradiation. Flow cytometric analysis showed that carbon ion irradiation induced a permanent G2/M arrest in PC3 cells at lower doses (2 Gy) compared to X-rays (5 Gy), while in Caco-2 cells the G2/M arrest was transient after irradiation with X-rays (2 and 5 Gy) but persistent after exposure to carbon ions (2 Gy).
机译:带电粒子束(例如碳离子)的使用正成为癌症治疗中越来越有吸引力的治疗选择。鉴于精确的吸收剂量定位和更高的生物学有效性,与传统的放射治疗相比,这种治疗形式更为有利,目前正用于治疗特定类型的癌症。粒子束的高弹道精度将最大剂量沉积在肿瘤上,而对周围健康组织的损害却受到限制。为了更好地了解导致生物学效力提高的潜在机制,我们研究了两种p53突变细胞系(更具体地是前列腺癌(PC3)和结肠癌(Caco-2)癌细胞)的DNA损伤和修复动力学以及细胞周期进程线,暴露于不同的辐射质量之后。在法国卡昂国家大离子实验室,用不同吸收剂量(0、0.5和2 0.5Gy)的加速的 13 C离子辐照细胞,或用X射线( 0、0.1、0.5、1、2和5 Gy)。 DNA双链断裂的显微镜分析显示,在两种细胞系中,暴露于两种类型的辐射后,γ-H2AX病灶数和病灶占有率呈剂量依赖性增加。然而,在暴露后24小时,与X射线相比,较低剂量的碳离子辐射后残留损伤更为明显。流式细胞仪分析表明,与X射线(5 Gy)相比,碳离子辐照以更低的剂量(2 Gy)在PC3细胞中引起G2 / M永久性阻滞,而在Caco-2细胞中,辐照后G2 / M阻滞是短暂的用X射线(2和5 Gy)照射,但在暴露于碳离子(2 Gy)后仍然存在。

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