Anne Van Arsdale, Olga Meshcheryakova, Sonia Gallego, Elaine Maggi, Bryan Harmon, Koenraad Van Doorslaer, Dennis YS Kuo, Mark H Einstein, Brian Haas, Cristina Montagna, Jack Lenz
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引用次数: 0
摘要
几乎所有宫颈癌都是由人类乳头瘤病毒(HPV)引起的。在大多数情况下,HPV DNA 会整合到人类基因组中。我们发现,在宫颈癌患者接受初次治疗时,其血清无细胞 DNA 中可检测到肿瘤特异性 HPV 与人类 DNA 连接。回顾性分析表明,在癌症后来复发的妇女中更经常检测到这些连接。我们还发现,在我们的研究和癌症基因组图谱(The Cancer Genome Atlas)宫颈癌数据库中,尽管包括 HPV16 在内的非 α9 型 HPV 在宫颈癌中的发病率较高,但由系统发育支系 α9 以外的 HPV 所导致的宫颈癌的复发率高于由 α9 型 HPV 所导致的宫颈癌。因此,检测血清无细胞DNA中的HPV-人类DNA接合点和确定肿瘤组织中的HPV类型可能有助于预测复发风险。筛查血清无细胞 DNA 中的接合点还可以提供一种明确、无创的方法来监测治疗后是否复发。
Serum, Cell-Free HPV-Human DNA Junction Detection and HPV Typing for Predicting and Monitoring Cervical Cancer Recurrence
Almost all cervical cancers are caused by human papillomaviruses (HPVs). In most cases, HPV DNA is integrated into the human genome. We found that tumor-specific, HPV-human DNA junctions are detectable in serum cell-free DNA of cervical cancer patients at initial treatment. Retrospective analysis revealed these junctions were more frequently detectable in women in whom the cancer later recurred. We also found that cervical cancers caused by HPV types outside of phylogenetic clade α9 had a higher recurrence frequency than those caused by α9 types in both our study and The Cancer Genome Atlas cervical cancer database, despite the higher prevalence of non-α9 types including HPV16 in cervical cancer. Thus, HPV-human DNA junction detection in serum cell-free DNA and HPV type determination in tumor tissue may help predict recurrence risk. Screening serum cell-free DNA for junctions may also offer an unambiguous, non-invasive means to monitor absence of recurrence following treatment.
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