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人乳头瘤病毒16型E2基因整合与宫颈癌无病生存期不佳的关联。

Association of human papillomavirus type 16 integration in the E2 gene with poor disease-free survival from cervical cancer.

作者信息

Vernon S D, Unger E R, Miller D L, Lee D R, Reeves W C

机构信息

Viral Exanthems and Herpesvirus Branch, National Center for Infectious Diseases, Centers for Disease Control and Prevention, Atlanta, GA 30333, USA.

出版信息

Int J Cancer. 1997 Feb 20;74(1):50-6. doi: 10.1002/(sici)1097-0215(19970220)74:1<50::aid-ijc9>3.0.co;2-#.

Abstract

To determine the clinical relevance of human papillomavirus (HPV) integration and E2 function suggested by in vitro studies, we investigated 50 patients with HPV 16-positive primary cervical carcinoma (stage Ib-IV) diagnosed and treated at one institution. The physical state of HPV was determined by colorimetric in situ hybridization and was not found to vary by stage. Overall, 62% of tumors had integrated HPV, 16% had episomal and 22% had both integrated and episomal. The E1/E2 region was evaluated by 8 separate polymerase chain reactions, which resulted in overlapping products. There was no significant variation in ability to amplify the E1/E2 region with stage. E1/E2 amplification correlated with physical state. Nearly all tumors with episomal or mixed HPV 16 DNA amplified all 8 E1/E2 fragments. Half of the tumors with integrated HPV 16 DNA failed to amplify one or more E1/E2 fragments. Disruptions were most frequent in the E2 region. For all 46 patients receiving curative therapy, the Kaplan-Meier estimate of disease-free survival was determined for those whose primary tumors had amplifiable E2 compared with those lacking one or more E2 DNA fragments. Disruption of E2 was associated with significantly shortened disease-free survival.

摘要

为了确定体外研究提示的人乳头瘤病毒(HPV)整合及E2功能的临床相关性,我们调查了在同一机构诊断并治疗的50例HPV 16阳性原发性宫颈癌(Ib-IV期)患者。通过比色原位杂交确定HPV的物理状态,且未发现其随分期而变化。总体而言,62%的肿瘤有整合型HPV,16%有游离型,22%既有整合型又有游离型。通过8个独立的聚合酶链反应评估E1/E2区域,这些反应产生重叠产物。E1/E2区域的扩增能力在分期上无显著差异。E1/E2扩增与物理状态相关。几乎所有有游离型或混合型HPV 16 DNA的肿瘤都扩增出了所有8个E1/E2片段。一半有整合型HPV 16 DNA的肿瘤未能扩增出一个或多个E1/E2片段。E2区域的破坏最为常见。对于所有接受根治性治疗的46例患者,对其原发性肿瘤有可扩增E2的患者与缺乏一个或多个E2 DNA片段的患者进行了无病生存期的Kaplan-Meier估计。E2的破坏与无病生存期显著缩短相关。

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