How virus persistence can initiate the tumorigenesis process

来源 :World Journal of Virology | 被引量 : 0次 | 上传用户:tsengyg
下载到本地 , 更方便阅读
声明 : 本文档内容版权归属内容提供方 , 如果您对本文有版权争议 , 可与客服联系进行内容授权或下架
论文部分内容阅读
Human oncogenic viruses are defined as necessary but not sufficient to initiate cancer. Experimental evidence suggests that the oncogenic potential of a virus is effective in cells that have already accumulated a number of genetic mutations leading to cell cycle deregulation. Current models for viral driven oncogenesis cannot explain why tumor development in carriers of tumorigenic viruses is a very rare event, occurring decades after virus infection. Considering that viruses are mutagenic agents per se and human oncogenic viruses additionally establish latent and persistent infections, we attempt here to provide a general mechanism of tumor initiation both for RNA and DNA viruses, suggesting viruses could be both necessary and sufficient in triggering human tumorigenesis initiation. Upon reviewing emerging evidence on the ability of viruses to induce DNA damage while subverting the DNA damage response and inducing epigenetic disturbance in the infected cell, we hypothesize a general, albeit inefficient hit and rest mechanism by which viruses may produce a limited reservoir of cells harboring permanent damage that would be initiated when the vi-rus first hits the cell, before latency is established. Cells surviving virus generated damage would consequently become more sensitive to further damage mediated by the otherwise insufficient transforming activity of virus products expressed in latency, or upon episodic reactivations(viral persistence). Cells with a combination of genetic and epigenetic damage leading to a cancerous phenotype would emerge very rarely, as the probability of such an occurrence would be dependent on severity and frequency of consecutive hit and rest cycles due to viral reinfections and reactivations. Experimental evidence suggests that the oncogenic potential of a virus is effective in cells that have already accumulated a number of genetic mutations leading to cell cycle deregulation. Current models for viral driven oncogenesis can not explain why tumor development in carriers of tumorigenic viruses is a very rare event, occurring attempt after after virus infection. initiation review for emerging viruses on both genotoxic and viral threats induce DNA damage while inducing epigenetic disturbance in the infected cells. we hypothesize a general, albeit inefficient hit and rest mechanism by which viruses may produce a limited reservoir of cells harboring permanent damage that would be initiated when the vi-rus first hits the cell, before latency is established. Cells surviving virus generated damage would not became more sensitive to further damage mediated by the otherwise less transforming activity of virus products expressed in latency, or upon episodic reactivations (viral persistence). Cells with a combination of genetic and epigenetic damage leading to a cancerous phenotype would emerge very rarely, as the probability of such an occurrence would be dependent on severity and frequency of consecutive hit and rest cycles due to viral reinfections and reactivations.
其他文献
期刊
期刊
抗菌肽是近年来研究发现的新一代抗菌剂,对机体免疫功能等具有重要作用。水生动物抗菌肽的相关研究起步较晚,本文初步研究黄鳝肝脏、肠道等组织粗提物的抗菌活性,在此基础上进一
期刊
肌肉生长抑制素(Myostatin)属于转化生长因子-β(TGF-β)超家族成员之一,又名为生长/分化因子-8(GDF-8)。Myostatin是在骨骼肌中广泛表达的一类糖蛋白,其作用特征是对肌肉生长有负
以陇东草原3种主要植物长芒草(Stipa bungeana)、达乌里胡枝子(Lespedezadavurica)和茵陈蒿(Artemisia.Capillaris)枯落物水提液为施体材料,根据不同放牧率样地、封育样地、
AIM: To study the expression of carbonic anhydrase(CA) 9 in human hepatocellular carcinoma(HCC) cells.METHODS: We studied CA9 protein, CA9 m RNA and hypoxia-ind
干旱环境下植物和水分的关系一直是植物生理与生态学领域研究的重点问题,植物根系提水作用研究在逐渐增多,而有关施肥对根系提水影响的研究报道较少。本实验采用上下桶分根法,通过向下桶施肥来研究施肥对沙打旺(Astragalus adsurgens)根系提水作用能力、沙打旺生理特性及上桶土壤养分活性的影响。主要结论如下:1.沙打旺根系提水量随施肥量的增加而增加;在上桶不浇水的情况下,高肥处理组上桶伴生的浅根
胚胎干细胞(Embryonic Stem Cells, ES细胞)是由动物附植前胚胎的内细胞团(Inner Cell Mass, ICM)经体外分离培养而建立的克隆细胞系。ES细胞是一种全能干细胞,具有与胚胎细胞相
Background: We examined the impact of adjuvant modalities on resected pancreatic and periampullary adenocarcinoma(PAC).Methods: A total of 563 patients who were