Genetic inhibition of autophagy in a transgenic mouse model of anal cancer.

Q1 Environmental Science Journal of Carcinogenesis Pub Date : 2018-07-23 eCollection Date: 2018-01-01 DOI:10.4103/jcar.JCar_4_18
Brooks L Rademacher, Louise M Meske, Kristina A Matkowskyj, Bret M Hanlon, Evie H Carchman
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引用次数: 5

Abstract

Background: The dynamic role of autophagy in cancer development is a topic of considerable research and debate. Previously published studies have shown that anal cancer development can be promoted or prevented with the pharmacologic inhibition or induction, respectively, of autophagy in a human papillomavirus (HPV) mouse model. However, these results are confounded by the fact that the drugs utilized are known to affect other pathways besides autophagy. It has also been shown that autophagic inhibition occurs in the setting of HPV16 oncoprotein expression (E6 and E7) and correlates with increased susceptibility to anal carcinogenesis.

Materials and methods: In this study, we employed a conditional, genetic, autophagic (Atg7) knockout mouse model to determine conclusively that autophagy has a role in anal cancer development, in the absence or presence of E6 and E7.

Results: In mice lacking both HPV16 oncogenes, knockout of autophagy followed by exposure to a carcinogen resulted in a tumor incidence of 40%, compared to 0% in mice treated with a carcinogen alone with an intact autophagic pathway (P = 0.007). In mice expressing either one or both HPV16 oncoproteins, the addition of genetic knockout of autophagy to carcinogen treatment did not lead to a significant difference in tumor incidence compared to carcinogen treatment alone, consistent with the ability of HPV oncogenes to inhibit autophagy in themselves.

Conclusions: These results provide the first conclusive evidence for the distinct role of autophagy in anal carcinogenesis, and suggest that autophagy is a plausible target for therapies aimed at reducing anal dysplasia and anal cancer development.

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转基因小鼠肛门癌自噬的基因抑制。
背景:自噬在癌症发展中的动态作用是一个相当多的研究和争论的话题。先前发表的研究表明,在人乳头瘤病毒(HPV)小鼠模型中,分别通过药物抑制或诱导自噬来促进或预防肛门癌的发展。然而,这些结果被这样一个事实所混淆,即所使用的药物已知会影响自噬之外的其他途径。研究还表明,自噬抑制发生在HPV16癌蛋白表达(E6和E7)的情况下,并与肛门癌易感性增加相关。材料和方法:在本研究中,我们采用条件、遗传、自噬(Atg7)敲除小鼠模型,最终确定在E6和E7缺失或存在的情况下,自噬在肛门癌的发展中起作用。结果:在缺乏两种HPV16癌基因的小鼠中,敲除自噬后暴露于致癌物导致肿瘤发生率为40%,而在完整自噬途径下单独使用致癌物治疗的小鼠中,肿瘤发生率为0% (P = 0.007)。在表达一种或两种HPV16癌蛋白的小鼠中,在致癌物治疗中加入自噬基因敲除并不会导致肿瘤发病率与单独致癌物治疗相比有显著差异,这与HPV癌基因自身抑制自噬的能力是一致的。结论:这些结果为自噬在肛门癌发生中的独特作用提供了第一个确凿的证据,并表明自噬是旨在减少肛门发育不良和肛门癌发展的治疗的合理目标。
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来源期刊
Journal of Carcinogenesis
Journal of Carcinogenesis Environmental Science-Health, Toxicology and Mutagenesis
CiteScore
7.50
自引率
0.00%
发文量
0
审稿时长
15 weeks
期刊介绍: Journal of Carcinogenesis considers manuscripts in many areas of carcinogenesis and Chemoprevention. Primary areas of interest to the journal include: physical and chemical carcinogenesis and mutagenesis; processes influencing or modulating carcinogenesis, such as DNA repair; genetics, nutrition, and metabolism of carcinogens; the mechanism of action of carcinogens and modulating agents; epidemiological studies; and, the formation, detection, identification, and quantification of environmental carcinogens. Manuscripts that contribute to the understanding of cancer prevention are especially encouraged for submission
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