非侵入性尿液标本中作为前列腺癌炎症辅助因子的高危人乳头瘤病毒存在的分子波动的研究

A. Kavrakova, B. Georgieva, K. Anachkov, K. Yanev, G. Ivanov, V. Mitev, A. Todorova
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引用次数: 0

摘要

背景:本研究的目的是通过PCA3、TMPRSS2-ERG融合和GSTP1启动子超甲基化来研究疑似前列腺癌(PCa)患者的无创尿液标本。此外,我们检测尿液标本中是否存在高风险的人乳头瘤病毒(HPV),作为前列腺癌(PCa)复杂起源的炎症辅助因子。方法:对50例有PSA升高和/或PCa生理症状的患者进行分析。RNA和DNA分离;反转录;实时聚合酶链反应;DNA测序;亚硫酸氢盐转化DNA;Methylationspecific PCR;进行细胞学准备和染色。结果:大多数患者均存在分子波动:肿瘤性GSTP1等位基因、PCA3强表达或高表达。仅有4例患者检测到TMPRSS2-ERG阳性。高危HPV类型在我们的尿液样本中检测到约35%,这些样本来自PCa高危患者,基于他们的分子谱。约96%的检测到的高危hpv分别为:16、33、35、31,分布在致癌潜力最高的亚群中。在尿路上皮感染的对照男性样本中,高危型HPV的估计频率明显较低(11%)。高危HPV阳性尿样细胞学切片病理检查显示炎症;细胞生长和分化的可变适应和部分病毒细胞病变效应。在部分分子PCa患者中,紊乱的癌前病变(原始细胞增加,成熟紊乱;细胞核增厚,染色质浓缩)。结论:我们的分子PCa的发现在细胞水平上得到了证实,细胞学表现为高度的改变:染色质结构分布粗糙,核膜不规则和增厚;高氮碳比;核仁突出,形状不规则;在一组细胞中存在相同的单一核仁(即“克隆”模式);肿瘤的素质。目前的研究涉及保加利亚PCa患者的新数据。
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Investigation of Noninvasive Urine Specimens with Molecular Fluctuations for a Presence of High-Risk Human Papilloma Viruses as an Inflammatory Cofactor in the Prostate Cancer
Background: The aim of the study is to investigate noninvasive urine specimens in suspected prostate cancer (PCa) patients by a panel of PCA3, TMPRSS2-ERG fusions and GSTP1 promoter hypermethylation. Furthermore, we tested urine specimens for the presence of high-risk Human Papilloma Viruses (HPV) as an inflammatory cofactor in the complicated origin of prostate cancer (PCa). Methods: A total of 50 patients with elevated PSA and/or PCa physiological symptoms were analyzed. RNA and DNA isolation; Reverse transcription; Real-time PCR; DNA sequencing; Bisulfite conversion of DNA; Methylationspecific PCR; Cytological preparations and staining were applied. Results: Molecular fluctuations were registered in most of the patients: neoplastic GSTP1 allele, PCA3 strongly elevated expression or hyperexpression. Only in 4 cases a positive TMPRSS2-ERG status was detected. High-risk HPV types were detected in ~ 35% of our urine specimens, obtained from patients at high risk of PCa based on their molecular profiles. Approximately 96% of detected high-risk HPVs are: 16, 33, 35, 31, distributed in the subgroup with highest oncogenic potential. The estimated frequency of high-risk HPV types in control male samples with urothelial infection is significantly lower (11%). The pathological examination on cytological slides from high-risk HPV positive urine specimens showed inflammation; variable adaptations of cellular growth and differentiation and partially viral cytopathic effect. In a proportion of patients with molecular PCa disturbed profile precancerous conditions (increased primitive cells with disturbed maturation; enlarged hyperchromatic nucleus and condensed chromatin) were found. Conclusion: Our molecular PCa findings, were confirmed on the cellular level with cytological findings of high grade alterations: coarse distributed chromatin texture with nuclear membrane irregularity and thickening; high N:C Ratio; prominence of nucleoli and irregularity in shape thereof; identical monotonous nucleoli present in all cells in a group (i.e., "Clonal" pattern); Tumor diathesis. The present study concerns novel data for Bulgarian PCa patients.
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