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首页> 外文期刊>Radiation Research: Official Organ of the Radiation Research Society >Low doses of radiation increase the latency of spontaneous lymphomas and spinal osteosarcomas in cancer-prone, radiation-sensitive Trp53 heterozygous mice
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Low doses of radiation increase the latency of spontaneous lymphomas and spinal osteosarcomas in cancer-prone, radiation-sensitive Trp53 heterozygous mice

机译:低剂量辐射会增加易患癌症,对辐射敏感的Trp53杂合小鼠的自发性淋巴瘤和脊柱骨肉瘤的潜伏期

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Mice heterozygous for Trp53 are radiation-sensitive and cancer-prone, spontaneously developing a variety of cancer types. Osteosarcomas in the spine lead to paralysis, while lymphomas lead rapidly to death, distinct events that provide objective measures of latency. The effects of a single low-dose (10 or 100 mGy), low-dose-rate (0.5 mGy/min) Co-60 gamma irradiation on lymphoma or spinal osteosarcoma frequency and latency, defined as time of death or of onset of paralysis, respectively, were examined. Compared to spontaneous lymphomas or to spinal osteosarcomas leading to paralysis in unexposed mice, an exposure of 7-8-week-old Trp53(+/-) mice to 10 or 100 mGy had no significant effect on tumor frequency, indicating no effect on tumor initiation. All tumors are therefore assumed to be of spontaneous origin. However, a 10-mGy exposure reduced the risk of both lymphomas and spinal osteosarcomas by significantly increasing tumor latency, indicating that the main in vivo effect of a low-dose exposure is a reduction in the rate at which spontaneously initiated cells progress to malignancy. The effect of this adaptive response persisted for the entire life span of all the animals that developed these tumors. Exposure to 100 mGy delayed lymphoma latency longer than the 10-mGy exposure. However, the 100-mGy dose increased spinal osteosarcoma risk by decreasing overall latency compared to unexposed control mice. That result suggested that this higher dose was in a transition zone between reduced and increased risk, but that the dose at which the transition occurs varies with the tumor type. (C) 2003 by Radiation Research Society. [References: 20]
机译:Trp53杂合的小鼠对辐射敏感且容易患癌症,自发发展为多种癌症类型。脊柱骨肉瘤会导致瘫痪,而淋巴瘤会迅速导致死亡,不同事件可客观地反映潜伏期。一次低剂量(10或100 mGy),低剂量率(0.5 mG​​y / min)Co-60γ射线照射对淋巴瘤或脊柱骨肉瘤的频率和潜伏期的影响,定义为死亡时间或麻痹发作时间分别进行了检查。与自发性淋巴瘤或脊柱骨肉瘤导致未暴露小鼠瘫痪相比,将7-8周龄的Trp53(+/-)小鼠暴露于10或100 mGy对肿瘤发生率没有明显影响,表明对肿瘤没有影响引发。因此,假定所有肿瘤都是自发性的。然而,10-mGy暴露通过显着增加肿瘤潜伏期而降低了淋巴瘤和脊柱骨肉瘤的风险,这表明低剂量暴露的主要体内效应是自发引发细胞发展为恶性肿瘤的速率降低。这种适应性反应的影响在所有罹患这些肿瘤的动物的整个生命周期中一直存在。暴露于100 mGy的延迟淋巴瘤潜伏期比暴露于10 mGy的更长。然而,与未暴露的对照小鼠相比,100-mGy剂量通过降低总体潜伏期而增加了脊柱骨肉瘤的风险。该结果表明,较高剂量处于风险降低和风险增加之间的过渡区域,但是发生过渡的剂量随肿瘤类型而变化。 (C)2003年,辐射研究学会。 [参考:20]

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