Copy Number Profiling Implicates Thin High-Grade Squamous Intraepithelial Lesions as a True Precursor of Cervical Human Papillomavirus-Induced Squamous Cell Cancer

IF 5.1 2区 医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL
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引用次数: 0

Abstract

Full-thickness high-grade squamous intraepithelial lesions (HSIL) are precursors of invasive cervical squamous cell carcinoma (SCC). The World Health Organization and Lower Anogenital Squamous Terminology Standardization Project for human papilloma virus (HPV)–associated lesions divide full-thickness HSIL of the cervix into thin HSIL with thickness of 1 to 9 cell layers and the typical full-thickness HSIL of >10 cell layers. Although HPV oncogene transcripts and p16ink4a overexpression, as markers of transforming HPV infection, are detectable in thin HSIL, the biological significance of thin HSIL in cervical carcinogenesis remains poorly understood. To further characterize thin HSIL, we performed a comparative study of chromosomal copy number variations (CNV), an analysis of dysregulated genes present in the segments with CNV, and a generalized genetic complexity calculation for 31 thin HSIL, 31 thick HSIL, 24 microinvasive SCC (pT1a SCC), and 22 highly invasive SCC samples. Thin HSIL share various CNV and specific dysregulated gene pathways with thick HSIL and invasive SCC. Thin HSIL exhibited an average CNV of 11.6% compared with 14.1% for thick HSIL, 15.5% for pT1a SCC, and 26.6% for highly invasive SCC. The CNV included gains at 1q and 3q (40% and 43%, respectively), partial loss of 3p, and loss of chromosomes 11 (18%), 16 (50%), 20 (35%), and 22 (40%). Pathways affected solely in thin HSIL were those enhancing immune evasion and primarily involved the (interleukin) IL6, IL21, and IL23 genes. ILs are transiently upregulated in response to infection and play a crucial role in mounting antitumor T-cell activity. Deregulation reflects an attempt by the HPV to evade the initial immune response of the host. The primary pathways shared by thick HSIL and invasive SCC were interactions between lymphoid and nonlymphoid cells, NOTCH2 signaling, tight junction interactions (primarily of the claudin family), and FGR2 alternative splicing. Our results show that thin HSIL carry similar genetic changes as thick HSIL and SCC, indicating that thin HSIL are true precursor lesions that can progress to thick HSIL and SCC.

拷贝数图谱显示,薄型高级别鳞状上皮内病变是宫颈人类乳头瘤病毒诱发鳞状细胞癌的真正前体。
全厚高级别鳞状上皮内病变(HSIL)是浸润性宫颈鳞状细胞癌(SCC)的前兆。世界卫生组织(WHO)和人乳头瘤病毒(HPV)相关病变的下生殖器鳞状术语(LAST)标准化项目将宫颈的全厚HSIL分为1至9个细胞层厚度的薄型HSIL和超过10个细胞层的典型全厚HSIL。虽然薄型 HSIL 中可以检测到作为转化型 HPV 感染标志物的 HPV 致癌基因转录本和 p16ink4a 过表达,但人们对薄型 HSIL 在宫颈癌发生过程中的生物学意义仍知之甚少。为了进一步描述薄型 HSIL 的特征,我们对 31 例薄型 HSIL、31 例厚型 HSIL、24 例微小浸润性 SCC(pT1a SCC)和 22 例高度浸润性 SCC 样本进行了染色体拷贝数变异(CNV)比较研究,分析了存在 CNV 的区段中的失调基因,并进行了广义遗传复杂性计算。薄型HSIL与厚型HSIL和浸润性SCC共享各种CNV和特定失调基因通路。薄型HSIL的CNV平均为11.6%,而厚型HSIL为14.1%,pT1a SCC为15.5%,高侵袭性SCC为26.6%。CNV 包括 1q 和 3q 的增益(分别为 40% 和 43%)、3p 的部分缺失以及 11 号染色体(18%)、16 号染色体(50%)、20 号染色体(35%)和 22 号染色体(40%)的缺失。仅在薄型 HSIL 中受影响的途径是那些增强免疫逃避的途径,主要涉及白细胞介素(IL)6、IL21 和 IL23 基因。ILs在感染时会短暂上调,并在启动抗肿瘤T细胞活性方面发挥关键作用。失调反映出 HPV 试图逃避宿主的初始免疫反应。厚HSIL和侵袭性SCC共有的主要途径是淋巴细胞和非淋巴细胞之间的相互作用、Notch2信号传导、紧密连接(TJ)相互作用(主要是claudin家族)和FGR2替代剪接。我们的研究结果表明,薄型HSIL与厚型HSIL和SCC具有相似的遗传变化,这表明薄型HSIL是真正的前驱病变,可发展为厚型HSIL和SCC。
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来源期刊
Laboratory Investigation
Laboratory Investigation 医学-病理学
CiteScore
8.30
自引率
0.00%
发文量
125
审稿时长
2 months
期刊介绍: Laboratory Investigation is an international journal owned by the United States and Canadian Academy of Pathology. Laboratory Investigation offers prompt publication of high-quality original research in all biomedical disciplines relating to the understanding of human disease and the application of new methods to the diagnosis of disease. Both human and experimental studies are welcome.
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