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首页> 外文期刊>Cancer biotherapy and radiopharmaceuticals >Low-dose-rate irradiation by 131I versus high-dose-rate external-beam irradiation in the rat pancreatic tumor cell line CA20948.
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Low-dose-rate irradiation by 131I versus high-dose-rate external-beam irradiation in the rat pancreatic tumor cell line CA20948.

机译:大鼠胰腺肿瘤细胞系CA20948中131I的低剂量率照射与高剂量率的外部束照射。

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AIM: The rat pancreatic CA20948 tumor cell line is widely used in receptor-targeted preclinical studies because many different peptide receptors are expressed on the cell membrane. The response of the tumor cells to peptide radionuclide therapy, however, is dependent on the cell line's radiosensitivity. Therefore, we measured the radiosensitivity of the CA20948 tumor cells by using clonogenic survival assays after high-energy external-beam radiotherapy (XRT) in vitro. It can, however, be expected that results of high-dose-rate XRT are not representative for those after low-dose-rate radionuclide therapy (RT), such as peptide-receptor radionuclide therapy. Therefore, we compared clonogenic survival in vitro in CA20948 tumor cells after increasing doses of XRT or RT, the latter using (131)I. METHODS: Survival of CA20948 cells was investigated using a clonogenic survival assay after RT by incubation with increasing amounts of (131)I, leading to doses of 1-10 Gy after 12 days of incubation (maximum dose rate, 0.92 mGy/min), or with doses of 1-10 Gy using an X-ray machine (dose rate, 0.66 Gy/min). Colonies were scored after a 12-day-incubation period. Also, the doubling time of this cell line was calculated. RESULTS: We observed a dose-dependent reduction in tumor-cell survival, which, at low doses, was similar for XRT and RT. For high-dose-rate XRT, the quadratic over linear component ratio (alpha/beta) for CA20948 was 8.3 Gy, whereas that ratio for low-dose-rate RT was calculated to be 86.5 Gy. The calculated doubling time of CA20948 cells was 22 hours. CONCLUSIONS: Despite the huge differences in dose rate, RT tumor cell-killing effects were approximately as effective as those of XRT at doses of 1 and 2 Gy, the latter being the common daily dose given in fractionated external-beam therapies. At higher doses, RT was less effective than XRT.
机译:目的:大鼠胰腺CA20948肿瘤细胞系广泛用于受体靶向的临床前研究,因为细胞膜上表达了许多不同的肽受体。然而,肿瘤细胞对肽放射性核素疗法的反应取决于细胞系的放射敏感性。因此,我们在体外高能束体外放射治疗(XRT)后,通过使用克隆形成存活测定法测量了CA20948肿瘤细胞的放射敏感性。但是,可以预期,高剂量率XRT的结果不能代表低剂量率放射性核素治疗(RT)(例如肽受体放射性核素治疗)后的结果。因此,我们比较了增加剂量的XRT或RT后CA20948肿瘤细胞在体外的克隆形成存活率,后者使用(131)I。方法:在RT后,通过与逐渐增加的(131)I孵育,使用克隆形成存活分析研究CA20948细胞的存活,孵育12天后产生1-10 Gy的剂量(最大剂量率,0.92 mGy / min),或使用X射线机剂量为1-10 Gy(剂量率,0.66 Gy / min)。培养12天后对菌落进行评分。同样,计算了该细胞系的倍增时间。结果:我们观察到肿瘤细胞生存的剂量依赖性降低,在低剂量时,XRT和RT相似。对于高剂量率XRT,CA20948的二次线性成分比率超过线性分量比(alpha / beta)为8.3 Gy,而低剂量率RT的比率为86.5 Gy。 CA20948细胞的计算倍增时间为22小时。结论:尽管剂量率存在巨大差异,但在1和2 Gy剂量下,RT肿瘤细胞杀伤效果与XRT相当,后者是分段外束疗法中常见的每日剂量。在较高剂量下,RT的疗效不如XRT。

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