首页> 美国卫生研究院文献>American Journal of Blood Research >Epstein-Barr virus-positive diffuse large B-cell lymphoma of the elderly expresses EBNA3A with conserved CD8+ T-cell epitopes
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Epstein-Barr virus-positive diffuse large B-cell lymphoma of the elderly expresses EBNA3A with conserved CD8+ T-cell epitopes

机译:EB病毒阳性的老年人弥漫性大B细胞淋巴瘤表达具有保守CD8 + T细胞表位的EBNA3A

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摘要

Post-transplantation lymphoproliferative disorders (PTLD) arise in the immunosuppressed and are frequently Epstein-Barr virus (EBV) associated. The most common PTLD histological sub-type is diffuse large B-cell lymphoma (EBV+DLBCL-PTLD). Restoration of EBV-specific T-cell immunity can induce EBV+DLBCL-PTLD regression. The most frequent B-cell lymphoma in the immunocompetent is also DLBCL. ‘EBV-positive DLBCL of the elderly’ (EBV+DLBCL) is a rare but well-recognized DLBCL entity that occurs in the overtly immunocompetent, that has an adverse outcome relative to EBV-negative DLBCL. Unlike PTLD (which is classified as viral latency III), literature suggests EBV+DLBCL is typically latency II, i.e. expression is limited to the immuno-subdominant EBNA1, LMP1 and LMP2 EBV-proteins. If correct, this would be a major impediment for T-cell immunotherapeutic strategies. Unexpectedly we observed EBV+DLBCL-PTLD and EBV+DLBCL both shared features consistent with type III EBV-latency, including expression of the immuno-dominant EBNA3A protein. Extensive analysis showed frequent polymorphisms in EB-NA1 and LMP1 functionally defined CD8+ T-cell epitope encoding regions, whereas EBNA3A polymorphisms were very rare making this an attractive immunotherapy target. As with EBV+DLBCL-PTLD, the antigen presenting machinery within lymphomatous nodes was intact. EBV+DLBCL express EBNA3A suggesting it is amenable to immunotherapeutic strategies.
机译:移植后的淋巴增生性疾病(PTLD)以免疫抑制的形式出现,并经常与爱泼斯坦-巴尔病毒(EBV)相关。 PTLD最常见的组织学亚型是弥漫性大B细胞淋巴瘤(EBV + DLBCL-PTLD)。恢复EBV特异性T细胞免疫可诱导EBV + DLBCL-PTLD退化。免疫功能最常见的B细胞淋巴瘤也是DLBCL。 “老年人EBV阳性DLBCL”(EBV + DLBCL)是一种罕见但广为人知的DLBCL实体,它发生在明显的免疫功能上,相对于EBV阴性DLBCL而言,其不良后果。与PTLD(分类为病毒潜伏期III)不同,文献表明EBV + DLBCL通常是潜伏期II,即表达仅限于免疫为主的EBNA1,LMP1和LMP2 EBV蛋白。如果正确,这将是T细胞免疫治疗策略的主要障碍。出乎意料的是,我们观察到EBV + DLBCL-PTLD和EBV + DLBCL都具有与III型EBV潜伏期一致的特征,包括表达免疫优势的EBNA3A蛋白。广泛的分析表明,EB-NA1和LMP1在功能上定义的CD8 + T细胞表位编码区中频繁出现多态性,而EBNA3A的多态性非常罕见,因此使其成为有吸引力的免疫治疗靶标。与EBV + DLBCL-PTLD一样,淋巴瘤淋巴结内的抗原呈递机制是完整的。 EBV + DLBCL表达EBNA3A,表明它适用于免疫治疗策略。

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