Atypical Epstein-Barr viral genomic structure in lymphoma tissue and lymphoid cell lines.

Weihua Tang, Hongxin Fan, Jane Schroeder, Cherie H Dunphy, Ronald J Bryant, Yuri Fedoriw, Margaret L Gulley
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引用次数: 8

Abstract

Epstein-Barr virus (EBV) DNA is found within the malignant cells of some subtypes of lymphoma, and viral presence is being exploited for improved diagnosis, monitoring, and management of affected patients. Recent work suggests that viral genomic polymorphism, such as partial deletion of the viral genome, could interfere with virus detection in tumor tissues. To test for atypical forms of the EBV genome, 98 lymphomas and 6 infected cell lines were studied using a battery of 6 quantitative polymerase chain reaction assays targeting disparate sections of EBV DNA. Fifty of the lymphomas (51%) had no amplifiable EBV DNA, and 38 lymphomas (39%) had low-level EBV infection that was deemed incidental based on EBV-encoded RNA (EBER) in situ hybridization results. The remaining 10 lymphomas (10%) had high EBV loads and EBER localization to malignant cells by EBER in situ hybridization. All 10 represented lymphoma subtypes were previously associated with EBV (Burkitt, diffuse large B-cell, or T-cell type), whereas no remnants of EBV were detected in other lymphoma subtypes (follicular, small lymphocytic, mantle cell, or marginal zone type). Interestingly, 4 of the 10 infected lymphomas had evidence of atypical viral genomes, including 3 of 4 infected T-cell lymphomas with aberrant loss of LMP2 amplicons, and a single diffuse large B-cell lymphoma lacking the central part of the viral genome spanning BamH1W, BZLF1, and EBNA1 gene segments. A reasonable screening strategy for infected malignancy involves applying EBER1 and LMP1 quantitative polymerase chain reaction assays and confirming that values exceeding 2000 copies of EBV per 100,000 cells have EBER localization to malignant cells.

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非典型eb病毒在淋巴瘤组织和淋巴样细胞系中的基因组结构。
eb病毒(EBV) DNA存在于某些淋巴瘤亚型的恶性细胞中,病毒的存在正被用于改善受影响患者的诊断、监测和管理。最近的研究表明,病毒基因组多态性,如病毒基因组的部分缺失,可能会干扰肿瘤组织中的病毒检测。为了检测EBV基因组的非典型形式,对98个淋巴瘤和6个感染细胞系进行了研究,使用了针对EBV DNA不同部分的6种定量聚合酶链反应试验。50个淋巴瘤(51%)没有可扩增的EBV DNA, 38个淋巴瘤(39%)有低水平的EBV感染,根据EBV编码RNA (EBER)原位杂交结果认为是偶然的。其余10例淋巴瘤(10%)EBV载量高,通过原位杂交发现其定位于恶性细胞。所有10种代表的淋巴瘤亚型先前都与EBV相关(Burkitt,弥漫性大b细胞或t细胞型),而在其他淋巴瘤亚型(滤泡型,小淋巴细胞型,套细胞型或边缘带型)中未检测到EBV的残余。有趣的是,10个感染淋巴瘤中有4个具有非典型病毒基因组的证据,包括4个感染t细胞淋巴瘤中的3个具有LMP2扩增子的异常缺失,以及单个弥漫性大b细胞淋巴瘤缺乏跨越BamH1W, BZLF1和EBNA1基因片段的病毒基因组的中心部分。感染恶性肿瘤的合理筛选策略包括应用EBER1和LMP1定量聚合酶链反应测定,并确认每10万个细胞中超过2000拷贝的EBV值表明EBER定位于恶性细胞。
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期刊介绍: Diagnostic Molecular Pathology focuses on providing clinical and academic pathologists with coverage of the latest molecular technologies, timely reviews of established techniques, and papers on the applications of these methods to all aspects of surgical pathology and laboratory medicine. It publishes original, peer-reviewed contributions on molecular probes for diagnosis, such as tumor suppressor genes, oncogenes, the polymerase chain reaction (PCR), and in situ hybridization. Articles demonstrate how these highly sensitive techniques can be applied for more accurate diagnosis.
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