Morioka Takamitsu, Miyoshi-Imamura Tomoko, Blyth Benjamin J, Kaminishi Mutsumi, Kokubo Toshiaki, Nishimura Mayumi, Kito Seiji, Tokairin Yutaka, Tani Shusuke, Murakami-Murofushi Kimiko, Yoshimi Naoki, Shimada Yoshiya, Kakinuma Shizuko
Radiation Effect Accumulation and Prevention Project, Fukushima Project Headquarters, National Institute of Radiological Sciences, Chiba, Japan; Radiobiology for Children's Health Program, Research Center for Radiation Protection, National Institute of Radiological Sciences, Chiba, Japan.
Cancer Sci. 2015 Mar;106(3):217-26. doi: 10.1111/cas.12591. Epub 2015 Feb 12.
Genetic, physiological and environmental factors are implicated in colorectal carcinogenesis. Mutations in the mutL homolog 1 (MLH1) gene, one of the DNA mismatch repair genes, are a main cause of hereditary colon cancer syndromes such as Lynch syndrome. Long-term chronic inflammation is also a key risk factor, responsible for colitis-associated colorectal cancer; radiation exposure is also known to increase colorectal cancer risk. Here, we studied the effects of radiation exposure on inflammation-induced colon carcinogenesis in DNA mismatch repair-proficient and repair-deficient mice. Male and female Mlh1(-/-) and Mlh1(+/+) mice were irradiated with 2 Gy X-rays when aged 2 weeks or 7 weeks and/or were treated with 1% dextran sodium sulfate (DSS) in drinking water for 7 days at 10 weeks old to induce mild inflammatory colitis. No colon tumors developed after X-rays and/or DSS treatment in Mlh1(+/+) mice. Colon tumors developed after DSS treatment alone in Mlh1(-/-) mice, and exposure to radiation prior to DSS treatment increased the number of tumors. Histologically, colon tumors in the mice resembled the subtype of well-to-moderately differentiated adenocarcinomas with tumor-infiltrating lymphocytes of human Lynch syndrome. Immunohistochemistry revealed that expression of both p53 and β-catenin and loss of p21 and adenomatosis polyposis coli proteins were observed at the later stages of carcinogenesis, suggesting a course of molecular pathogenesis distinct from typical sporadic or colitis-associated colon cancer in humans. In conclusion, radiation exposure could further increase the risk of colorectal carcinogenesis induced by inflammation under the conditions of Mlh1 deficiency.
遗传、生理和环境因素与结直肠癌的发生有关。mutL同源蛋白1(MLH1)基因是DNA错配修复基因之一,该基因突变是遗传性结肠癌综合征(如林奇综合征)的主要原因。长期慢性炎症也是一个关键风险因素,可导致与结肠炎相关的结直肠癌;已知辐射暴露也会增加患结直肠癌的风险。在此,我们研究了辐射暴露对DNA错配修复功能正常和缺陷小鼠炎症诱导的结肠癌发生的影响。对2周龄或7周龄的雄性和雌性Mlh1(-/-)和Mlh1(+/+)小鼠进行2 Gy X射线照射,和/或在10周龄时用1%葡聚糖硫酸钠(DSS)处理饮用水7天以诱导轻度炎症性结肠炎。Mlh1(+/+)小鼠在接受X射线和/或DSS处理后未发生结肠肿瘤。Mlh1(-/-)小鼠单独接受DSS处理后发生了结肠肿瘤,在DSS处理前暴露于辐射会增加肿瘤数量。组织学上,小鼠的结肠肿瘤类似于人类林奇综合征中分化良好至中等的腺癌亚型,并伴有肿瘤浸润淋巴细胞。免疫组织化学显示,在致癌后期观察到p53和β-连环蛋白的表达以及p21和腺瘤性息肉病大肠杆菌蛋白的缺失,这表明其分子发病机制不同于人类典型的散发性或与结肠炎相关的结肠癌。总之,在Mlh1缺陷的情况下,辐射暴露会进一步增加炎症诱导的结直肠癌发生风险。
