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Analysis of carcinogenic mechanisms of liver cancers induced by chronic exposure to alpha-particles from internally deposited Thorotrast

机译:长期暴露于内部沉积的Thorotrast的α-颗粒诱导的肝癌致癌机制分析

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For the successful space traveling, the possibility for the detrimental effects on health including cancer caused by exposure to cosmic rays is a major concern. Thorotrast is a 25% colloidal solution of natural alpha-emitter, thorium dioxide used as a radiological contrast medium during World War II. It caused hepatic malignant tumors by the local exposure to alpha-particles decades after administration. Thorotrast-induced liver tumors consist of hepatocellular carcinoma (HCC), intrahepatic cholangiocarcinoma (ICC), and angiosarcoma (AS) at nearly the same instance. We analyzed mutations of the p53 and the K-ras genes, microsatellite instability (MSI), and loss of heterozygosity (LOH) in Thorotrast ICC. The major p53 mutation observed in Thorotrast ICC was the transition type, suggesting that reactive oxygen species are not likely involved in gene mutations of Thorotrast cancers. MSI frequency in Thorotrast ICC was significantly higher than that in non-Thorotrast ICC. MSI was partly attributed to the inactivation of the hMLH1 mismatch repair gene via methylation of the promoter region and to monoclonal expansion of cells with mutations. Thorotrast ICC shared LOH pattern with non-Thorotrast HCC and ICC. Furthermore, we could assess the distribution and the quantity of deposited thorium using an imaging plate and a BAS image analyzer. The distribution of thorium deposits was not always consistent with that of apoptotic cells. We conclude that Thorotrast ICC is developed through complex carcinogenic steps including genomic instability and mutations of crucial genes during remodeling of the liver architecture. We emphasize how pathological specimens from Thorotrast patients are valuable for assessing the relevance of long-term exposure to low dose a-particles to radiation carcinogenesis. (c) 2006 Elsevier Ltd. All rights reserved.
机译:对于成功的太空旅行,对健康的有害影响(包括因暴露于宇宙射线引起的癌症)的可能性是一个主要问题。 Thorotrast是天然α-发射体(二氧化th)的25%胶体溶液,在第二次世界大战期间用作放射造影剂。在给药后数十年,局部暴露于α-颗粒导致了肝恶性肿瘤。胸腔镜诱发的肝肿瘤几乎由同一情况下的肝细胞癌(HCC),肝内胆管癌(ICC)和血管肉瘤(AS)组成。我们分析了Thorotrast ICC中p53和K-ras基因的突变,微卫星不稳定性(MSI)和杂合性丧失(LOH)。在Thorotrast ICC中观察到的主要p53突变是过渡型,这表明活性氧不太可能与Thorotrast癌症的基因突变有关。 Thorotrast ICC中的MSI频率显着高于非Thorotrast ICC中的MSI频率。 MSI部分归因于通过启动子区域的甲基化使hMLH1错配修复基因失活以及具有突变的细胞的单克隆扩增。 Thorotrast ICC与非Thorotrast HCC和ICC共享LOH模式。此外,我们可以使用成像板和BAS图像分析仪评估th的分布和沉积量。 or沉积物的分布并不总是与凋亡细胞的分布一致。我们得出的结论是,Thorotrast ICC是通过复杂的致癌步骤开发的,包括基因组不稳定性和肝脏结构重塑过程中关键基因的突变。我们强调Thorotrast患者的病理学标本对于评估长期暴露于低剂量a粒子与放射致癌性之间的相关性是有价值的。 (c)2006 Elsevier Ltd.保留所有权利。

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