N,N'-二亚硝基哌嗪对TgN(p53mt-LMP1)/HT小鼠鼻腔和/或鼻咽上皮诱发癌前病变的增强作用。
Enhancive effect of N,N'-dinitrosopiperazine on inducing precancerous lesion on nasal and/or nasopharyngeal epithelia of TgN(p53mt-LMP1)/HT mice.
作者信息
Tian Dao-fa, He Ying-chun, Lu Fang-guo, Tang Fa-qing
机构信息
Faculty of Integrative Medicine, Chinese Medicine University of Hunan, and Department of Clinical Laboratory, the First Xiangya Hospital, Changsha 410007, China.
出版信息
J Zhejiang Univ Sci B. 2009 Mar;10(3):172-9. doi: 10.1631/jzus.B0820186.
OBJECTIVE
To investigate the enhancive effect of N,N'-dinitrosopiperazine (DNP) on induced carcinogenesis in nasal and/or nasopharyngeal epithelia among TgN(p53mt-LMP1)/HT transgenic mice to examine the underlying mechanism for the development of nasopharyngeal carcinoma (NPC).
METHODS
TgN(p53mt-LMP1)/HT transgenic mice and the same strain of C(57)BL/6J wild-type mice both at the age of 5 months were randomly divided into 2 groups in parallel, respectively, i.e., TgN(p53mt-LMP1)/HT cancerous lesion-inducing group (TI), TgN(p53mt-LMP1)/HT control group (TC), C57BL/6J cancerous lesion-inducing group (CI), and C57BL/6J control group (CC). TI and CI mice were treated only with DNP for 16 weeks, twice each week, while TC and CC mice were given the same volume of saline as controls. At the end of treatment, animals were sacrificed to collect epithelial tissue samples from nasal cavity and nasopharynx for pathohistological evaluation by haematoxylin and eosin (HE) staining and for determination on the expression of TRAF2, c-Jun, and p16 by immunohistochemistry.
RESULTS
Atypical hyperplasia was more significant in the samples of TI than in those of TC, CI, and CC, with the rates of lesions being 90%, 10%, 0, and 0 (P<0.01) respectively, though DNP was used alone in a much shortened inducing period at less dosage and without the use of carcinogenic promoter 12-O-tetradecanoylphorbol-13-acetate as usual. The expressions of tumor necrosis factor (TNF) receptor-associated factor 2 (TRAF2) and c-Jun in these samples were significantly up-regulated in TI (P<0.01), while the expression of p16 was significantly lower in TI than in the other groups (P<0.01).
CONCLUSION
TgN(p53mt-LMP1)/HT mice hold inherited constitutional defect in immune surveillance function, which can be aggravated by environmental carcinogens, such as DNP used even though in a much less strength. The enhanced carcinogenesis-inducing effect of DNP on TgN(p53mt-LMP1)/HT mice should be closely associated with abnormal signaling of activator protein-1 (AP-1) pathway, especially up-regulated expressions of TRAF2 and c-Jun, and down-regulated expression of p16.
目的
研究N,N'-二亚硝基哌嗪(DNP)对TgN(p53mt-LMP1)/HT转基因小鼠鼻和/或鼻咽上皮诱导致癌作用的增强效应,以探讨鼻咽癌(NPC)发生发展的潜在机制。
方法
将5月龄的TgN(p53mt-LMP1)/HT转基因小鼠和同品系的C(57)BL/6J野生型小鼠分别随机平行分为2组,即TgN(p53mt-LMP1)/HT癌前病变诱导组(TI)、TgN(p53mt-LMP1)/HT对照组(TC)、C57BL/6J癌前病变诱导组(CI)和C57BL/6J对照组(CC)。TI组和CI组小鼠仅用DNP处理16周,每周2次,而TC组和CC组小鼠给予相同体积的生理盐水作为对照。处理结束时,处死动物,收集鼻腔和鼻咽的上皮组织样本,进行苏木精-伊红(HE)染色的病理组织学评估,并通过免疫组织化学法测定TRAF2、c-Jun和p16的表达。
结果
TI组样本中的非典型增生比TC组、CI组和CC组更显著,病变率分别为90%、10%、0和0(P<0.01),尽管单独使用DNP时诱导期大大缩短,剂量更小,且未像往常那样使用致癌促进剂12-O-十四烷酰佛波醇-13-乙酸酯。这些样本中肿瘤坏死因子(TNF)受体相关因子2(TRAF2)和c-Jun的表达在TI组中显著上调(P<0.01),而p16的表达在TI组中显著低于其他组(P<0.01)。
结论
TgN(p53mt-LMP1)/HT小鼠在免疫监视功能方面存在遗传性体质缺陷,环境致癌物如DNP即使强度小得多也可使其加重。DNP对TgN(p53mt-LMP1)/HT小鼠致癌作用的增强效应应与激活蛋白-1(AP-1)途径的异常信号传导密切相关,尤其是TRAF2和c-Jun的上调表达以及p16的下调表达。
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