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首页> 外文期刊>Digestive Diseases and Sciences >Presence of JC virus DNA in the tumor tissue and normal mucosa of patients with sporadic colorectal cancer (CRC) or with positive family history and Bethesda criteria
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Presence of JC virus DNA in the tumor tissue and normal mucosa of patients with sporadic colorectal cancer (CRC) or with positive family history and Bethesda criteria

机译:散发性结直肠癌(CRC)或家族史和贝塞斯达标准阳性患者的肿瘤组织和正常黏膜中存在JC病毒DNA

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摘要

Introduction: JC virus (JCV) may infect the gastrointestinal tract in childhood, and, by encoding a gene for T-antigen (T Ag), can initiate chromosomal instability in epithelial cells. Aim: We looked for JCV DNA in the cancer tissue of patients with sporadic colorectal cancer (CRC, Group A) and with positive family history and Bethesda criteria (Group B). We hypothesized that the role of JCV may be different between these two groups. Methods: Fifty-six patients were randomly selected from our database, 30 in Group A and 26 in Group B. DNA was isolated from the tumor, normal mucosa, and plasma, and JCV DNA sequences were looked for with specific polymerase chain reaction (PCR) assays for T Ag primers. Immunohistochemistry for hMLH1, hMSH2, hMSH6, and PMS2 was performed on paraffin-embedded tissue. Results: In Group A, T Ag was demonstrated in 6 (20.00%) and 3 (10.00%) of the tumors and adjacent normal mucosa, respectively (P = 0.094). In Group B, the corresponding observations were 10 (38.46%) and 6 (23.07%), respectively (P < 0.001). Immunohistochemistry for hMLH1, hMSH2, hMSH6, and PMS2 was performed in all of the Group A and B patients. All patients of Group A (100%) showed expression of these proteins, while only 19 patients of Group B did so (73.1%), P = 0.009. JCV T Ag DNA was found in 20, 28.5, and 42.1% of the tumors in Group A, Group B with negative staining for DNA repair genes, and Group B with a positive staining, respectively (NS). Conclusion: CRC patients with positive family history have a higher incidence of JCV T Ag, but this did not correlate with specific DNA repair gene mutations. We could not conclude that, on the background of genetic mutation in one of the DNA repair genes, JCV acts as the missing link in the chain of events leading to CRC.
机译:简介:JC病毒(JCV)可能会感染儿童的胃肠道,并且通过编码T抗原(T Ag)的基因,可以引发上皮细胞的染色体不稳定。目的:我们在散发性结直肠癌(CRC,A组),家族史和贝塞斯达标准为阳性(B组)的患者的癌组织中寻找JCV DNA。我们假设在这两个小组之间,JCV的作用可能有所不同。方法:从我们的数据库中随机选择56例患者,A组30例,B组26例。从肿瘤,正常粘膜和血浆中分离DNA,并通过特异性聚合酶链反应(PCR)查找JCV DNA序列)检测T Ag引物。 hMLH1,hMSH2,hMSH6和PMS2的免疫组织化学在石蜡包埋的组织上进行。结果:在A组中,分别在6例(20.00%)和3例(10.00%)的肿瘤和邻近的正常粘膜中证实了T Ag(P = 0.094)。在B组中,相应的观察分别为10(38.46%)和6(23.07%)(P <0.001)。 A组和B组的所有患者均进行了hMLH1,hMSH2,hMSH6和PMS2的免疫组织化学分析。 A组的所有患者(100%)都显示了这些蛋白的表达,而B组中只有19个患者(73.1%)表达了这些蛋白,P = 0.009。 JCV T Ag DNA分别在A组,B组的DNA修复基因染色为阴性,B组的染色为阳性(NS)的肿瘤中分别占20%,28.5%和42.1%。结论:具有阳性家族史的CRC患者JCV T Ag的发生率较高,但这与特定的DNA修复基因突变无关。我们不能得出这样的结论,在DNA修复基因之一的基因突变的背景下,JCV成为导致CRC的事件链中缺失的环节。

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