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常见脆性位点是宫颈癌中HPV16整合的优先靶点。

Common fragile sites are preferential targets for HPV16 integrations in cervical tumors.

作者信息

Thorland Erik C, Myers Shannon L, Gostout Bobbie S, Smith David I

机构信息

Department of Biochemistry and Molecular Biology Mayo Clinic, Rochester, MN 55905, USA.

出版信息

Oncogene. 2003 Feb 27;22(8):1225-37. doi: 10.1038/sj.onc.1206170.

Abstract

The development of cervical cancer is highly associated with human papillomavirus (HPV) infection. HPV integration into the genome of infected cervical cells is temporally associated with the acquisition of the malignant phenotype. A relationship between the sites of HPV integration in cervical cancer and the position of the common fragile sites (CFSs) has been observed at both the cytogenetic and molecular levels. To further explore this relationship at the molecular level, we used RS-PCR to rapidly isolate cellular sequences flanking the sites of HPV16 integration in 26 primary cervical tumors. Human bacterial artificial chromosome clones were isolated based on these flanking sequences and used as probes for fluorescence in situ hybridization on aphidicolin-stimulated metaphases. Our data demonstrate that 11/23 HPV16 integrations in cervical tumors occurred within CFSs (P&<0.001). In addition, we show that deletions and complex rearrangements frequently occur in the cellular sequences targeted by the integrations and that integrations cluster in FRA13C (13q22), FRA3B (3p14.2), and FRA17B (17q23). Finally, our data suggest that cellular genes, such as Notch 1, are disrupted by the HPV16 integrations, which may contribute to the malignant phenotype.

摘要

宫颈癌的发生与人类乳头瘤病毒(HPV)感染高度相关。HPV整合到受感染宫颈细胞的基因组中与恶性表型的获得在时间上相关。在细胞遗传学和分子水平上均已观察到宫颈癌中HPV整合位点与常见脆性位点(CFSs)位置之间的关系。为了在分子水平上进一步探究这种关系,我们使用RS-PCR快速分离了26例原发性宫颈肿瘤中HPV16整合位点两侧的细胞序列。基于这些侧翼序列分离出人类细菌人工染色体克隆,并将其用作在阿非科林刺激的中期进行荧光原位杂交的探针。我们的数据表明,宫颈肿瘤中23例HPV16整合事件中有11例发生在CFSs内(P<0.001)。此外,我们发现整合靶向的细胞序列中经常发生缺失和复杂重排,并且整合聚集在FRA13C(13q22)、FRA3B(3p14.2)和FRA17B(17q23)中。最后,我们的数据表明,Notch 1等细胞基因会因HPV16整合而被破坏,这可能有助于形成恶性表型。

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