分析中低收入国家宫颈癌的进展情况:从恶性前病变到浸润性疾病。

IF 4.7 Q1 VIROLOGY Tumour Virus Research Pub Date : 2024-12-12 DOI:10.1016/j.tvr.2024.200299
Emma Robinson , Isabel Rodriguez , Victor Argueta , Yi Xie , Hong Lou , Rose Milano , Hyo Jung Lee , Laurie Burdett , Sambit K. Mishra , Meredith Yeager , Lisa Mirabello , Michael Dean , Roberto Orozco
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引用次数: 0

摘要

为了更好地了解宫颈癌的发展过程,我们分析了 262 例阴道镜检查妇女活组织切片的 RNA。我们确定了 HPV 类型,并分析了 51 个基因的表达。在癌前病变中,HPV31 的发病率明显高于 1 期癌症和浸润性癌症(P < 0.0001),而在浸润性疾病中,HPV16 的发病率则有所上升(P < 0.0001)。与HPV31癌前病变相比,CCNE1、MELTF和ULBP2在HPV16阳性癌前病变中明显增加,而NECTIN2和HLA-E的表达则有所减少。先天免疫系统标记物、DNA 修复基因和细胞周期基因在癌症进展过程中明显增加(p = 0.0001)。相比之下,TP53 和 RB1 抑癌基因在癌细胞中的表达明显减少。癌细胞中 T 细胞标志物 CD28 和 FLT3LG 表达减少,而 FOXP3、IDO1 和 ULBP2 表达增加。CD28 (p = 0.0005)、FOXP3 (p = 0.0002)、IDO1 (p = 0.038)、FLT3LG (p = 0.026)、APOBEC3B (p = 0.0011) 和 RUNX3 (p = 0.019)表达增加的个体生存率明显较高,而 ULBP2 表达增加的个体生存率明显较低 (p = 0.035)。这些结果将有助于我们阐明影响宫颈癌前病变向癌症发展的分子因素。了解特定 HPV 类型和亚系的进展风险有助于对阳性患者进行分流,而更好地了解免疫反应有助于开发和应用免疫疗法。
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Analysis of the progression of cervical cancer in a low-and-middle-income country: From pre-malignancy to invasive disease
To better understand cervical cancer progression, we analyzed RNA from 262 biopsies from women referred for colposcopy. We determined the HPV type and analyzed the expression of 51 genes. HPV31 was significantly more prevalent in precancer than stage 1 cancer and invasive cancer (p < 0.0001), and HPV16 increased in invasive disease (p < 0.0001). CCNE1, MELTF, and ULBP2 were significantly increased in HPV16-positive compared to HPV31 precancers, while NECTIN2 and HLA-E expression decreased. Markers of the innate immune system, DNA repair genes, and cell cycle genes are significantly increased during cancer progression (p = 0.0001). In contrast, the TP53 and RB1 tumor suppressor gene expression is significantly decreased in cancer cells. The T cell markers CD28 and FLT3LG expression decreased in cancer while FOXP3, IDO1, and ULBP2 expression increased. There is a significantly higher survival rate in individuals with increased expression of CD28 (p = 0.0005), FOXP3 (p = 0.0002), IDO1 (p = 0.038), FLT3LG (p = 0.026), APOBEC3B (p = 0.0011), and RUNX3 (p = 0.019), and a significantly lower survival rate in individuals with increased expression of ULBP2 (p = 0.035). These results will help us elucidate the molecular factors influencing the progression of cervical precancer to cancer. Understanding the risk of progression of specific HPV types and sublineages may aid in the triage of positive patients, and better knowledge of the immune response may aid in developing and applying immunotherapies.
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来源期刊
Tumour Virus Research
Tumour Virus Research Medicine-Infectious Diseases
CiteScore
6.50
自引率
2.30%
发文量
16
审稿时长
56 days
期刊最新文献
How can HPV E6 manipulate host cell differentiation process to maintain the reservoir of infection Rapid-onset cancer Too many cooks in the kitchen: HPV driven carcinogenesis – The result of collaboration or competition? Editorial: Tumour Virus Research on Virus Host Interactions and Cell Transformation. Drugs and drug targets for the treatment of HPV-positive cervical cancer
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