Loss of HPV16 E2 Protein Expression Without Disruption of the E2 ORF Correlates with Carcinogenic Progression.

The Open Virology Journal Pub Date : 2012-01-01 Epub Date: 2012-12-28 DOI:10.2174/1874357901206010163
Yuezhen Xue, Diana Lim, Liang Zhi, Pingping He, Jean-Pierre Abastado, Françoise Thierry
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引用次数: 32

Abstract

Integration of the viral DNA in the cellular genome has been suggested to be critical in carcinogenic progression of HPV-associated cervical neoplasia. This event can be accompanied by disruption of the open reading frame (ORF) encoding the E2 repressor, thus leading to transcriptional up-regulation of the E6 and E7 viral oncogenes. At this stage, it is unclear whether disruption of the E2 ORF is mandatory for carcinogenic progression. We measured E2 RNA and protein expression in clinical samples of various grades of HPV16-associated cervical neoplasia and compared it with the status of the viral genome. RNA extracted from paraffin embedded tissues was hybridized to specific probes and quantified by the NanoString technology. Protein expression was appreciated by immunohistochemistry and the status of viral DNA was determined by in situ hybridization, all performed on serial sections of the same samples. E2 protein was found highly expressed in CIN1, CIN2 lesions where the HPV DNA was highly replicative, while it was decreased in more advanced grade lesions where replication is decreased or lost (CIN3 and SCC). In contrast, E2 transcripts could be elevated even in conditions of no or low expression of the protein, as found in the Caski cell line. Our data demonstrate that integration of the viral DNA in the cellular genome does not always lead to disruption of the E2 ORF and drastic reduction of E2 transcripts, while in contrast, expression of the E2 protein is always drastically reduced.

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hpv16e2蛋白表达缺失而不破坏E2 ORF与致癌进展相关
病毒DNA在细胞基因组中的整合被认为是hpv相关宫颈肿瘤癌变进展的关键。这一事件可能伴随着编码E2抑制因子的开放阅读框(ORF)的破坏,从而导致E6和E7病毒癌基因的转录上调。在这个阶段,尚不清楚E2 ORF的破坏是否是致癌进展的强制性条件。我们测量了不同级别hpv16相关宫颈肿瘤临床样本中E2 RNA和蛋白的表达,并将其与病毒基因组的状态进行了比较。将从石蜡包埋组织中提取的RNA与特异性探针杂交,并利用NanoString技术进行定量分析。免疫组织化学检测蛋白表达,原位杂交检测病毒DNA状态,所有这些都是在同一样品的连续切片上进行的。E2蛋白在HPV DNA高度复制的CIN1, CIN2病变中被发现高表达,而在复制减少或丢失的更高级病变中被发现低表达(CIN3和SCC)。相反,在Caski细胞系中发现,即使在蛋白不表达或低表达的情况下,E2转录本也可以升高。我们的数据表明,病毒DNA在细胞基因组中的整合并不总是导致E2 ORF的破坏和E2转录物的急剧减少,相反,E2蛋白的表达总是急剧减少。
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