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爱泼斯坦-巴尔病毒相关胃癌及胃的爱泼斯坦-巴尔病毒感染

Epstein-Barr virus-associated gastric carcinoma and Epstein-Barr virus infection of the stomach.

作者信息

Fukayama M, Hayashi Y, Iwasaki Y, Chong J, Ooba T, Takizawa T, Koike M, Mizutani S, Miyaki M, Hirai K

机构信息

Department of Pathology, Tokyo Metropolitan Komagome Hospital, Japan.

出版信息

Lab Invest. 1994 Jul;71(1):73-81.

PMID:8041121
Abstract

BACKGROUND

Epstein-Barr virus (EBV) has been found to be associated with a type of gastric carcinoma (EBVaGC). However, many questions remain unanswered, such as epidemiology, and pathologic features of EBVaGC and the significance of EBV in the genesis of EBVaGC.

EXPERIMENTAL DESIGN

Gastric carcinoma and non-neoplastic mucosa were evaluated to reveal the following issues: the incidence of EBVaGC in Japanese population, pathologic features and EBV genotype, clonality, and gene-expression in EBVaGC, localization of EBV in non-neoplastic stomach, and serum titer of anti-EBV antibodies in EBVaGC-carrying patients.

RESULTS

Using PCR and EBER1 in situ hybridization, EBVaGC (definitely amplifiable EBV-DNA and positive EBER1-signal in the nuclei of carcinoma cells) was found in 8 of 72 gastric carcinomas (11%). The dominant genotype of EBV was type A (7/8), with type C (6/8), and F (8/8) restriction enzyme polymorphism, which are the predominant type of EBV found in throat washing of the general population in Japan. EBVaGC was found in the cardia (4/8) or body (4/8) of the stomach, and consisted of 7 advanced and 1 intramucosal carcinoma. By Southern blot analysis of EBVaGC hybridized with right- and left-side probe adjacent to the terminal repeats, EBV was present in a monoclonal episomal form in all of the EBVaGC. EBVaGC lacked expression of EBNA2 (0/8) and LMP1 (0/8) by immunocytochemistry. In non-neoplastic mucosa, EBER1 signal was identified in the infiltrating lymphocytes and shedding epithelial cells predominantly in fundic gland mucosa of patients with EBVaGC (8/8). Patients with EBVaGC showed high titers of anti-VCA IgG (8/8), anti-VCA IgA (2/8) and anti-EA IgG (7/8) antibodies just before surgery.

CONCLUSIONS

EBV may infect the surface epithelium of the stomach through the reactivated EBV-carrying lymphocytes. EBV may be a factor initiating EBVaGC. Anti-EBV antibodies or EBER1 in situ hybridization may help to identify patients at high risk for EBVaGC.

摘要

背景

已发现爱泼斯坦-巴尔病毒(EBV)与一种胃癌(EBV相关胃癌,EBVaGC)有关。然而,许多问题仍未得到解答,如EBVaGC的流行病学、病理特征以及EBV在EBVaGC发生中的意义。

实验设计

对胃癌组织和非肿瘤性黏膜进行评估,以揭示以下问题:日本人群中EBVaGC的发病率、病理特征和EBV基因型、克隆性以及EBVaGC中的基因表达、EBV在非肿瘤性胃中的定位,以及携带EBVaGC患者的抗EBV抗体血清滴度。

结果

采用聚合酶链反应(PCR)和EBER1原位杂交技术,在72例胃癌中有8例(11%)检测到EBVaGC(癌细胞核中EBV-DNA可明确扩增且EBER1信号呈阳性)。EBV的主要基因型为A型(7/8),具有C型(6/8)和F型(8/8)限制性酶切多态性,这是在日本普通人群咽拭子中发现的EBV主要类型。EBVaGC见于胃贲门部(4/8)或胃体部(4/8),包括7例进展期癌和1例黏膜内癌。通过与末端重复序列相邻的右侧和左侧探针杂交对EBVaGC进行Southern印迹分析,发现所有EBVaGC中的EBV均以单克隆游离形式存在。免疫细胞化学检测显示EBVaGC缺乏EBNA2(0/8)和LMP1(0/8)的表达。在非肿瘤性黏膜中,主要在EBVaGC患者胃底腺黏膜的浸润淋巴细胞和脱落上皮细胞中检测到EBER1信号(8/8)。EBVaGC患者在手术前抗VCA IgG(8/8)、抗VCA IgA(2/8)和抗EA IgG(7/8)抗体滴度较高。

结论

EBV可能通过重新激活的携带EBV的淋巴细胞感染胃表面上皮。EBV可能是引发EBVaGC的一个因素。抗EBV抗体或EBER1原位杂交可能有助于识别EBVaGC高危患者。

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