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Comprehensive Transcriptome and Mutational Profiling of Endemic Burkitt Lymphoma Reveals EBV Type-specific Differences

机译:全面的转录组和地方性伯基特淋巴瘤的突变谱揭示了EBV类型特异性的差异。

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摘要

Endemic Burkitt lymphoma (eBL) is the most common pediatric cancer in malaria-endemic equatorial Africa and nearly always contains Epstein-Barr virus (EBV), unlike sporadic Burkitt Lymphoma (sBL) that occurs with a lower incidence in developed countries. Given these differences and the variable clinical presentation and outcomes, we sought to further understand pathogenesis by investigating transcriptomes using RNA sequencing (RNAseq) from multiple primary eBL tumors compared to sBL tumors. Within eBL tumors, minimal expression differences were found based on: anatomical presentation site, in-hospital survival rates, and EBV genome type; suggesting that eBL tumors are homogeneous without marked subtypes. The outstanding difference detected using surrogate variable analysis was the significantly decreased expression of key genes in the immunoproteasome complex (PSMB9/β1i, PSMB10/β2i, PSMB8/β5i, and PSME2/PA28β) in eBL tumors carrying type 2 EBV compared to type 1 EBV. Secondly, in comparison to previously published pediatric sBL specimens, the majority of the expression and pathway differences was related to the PTEN/PI3K/mTOR signaling pathway and was correlated most strongly with EBV status rather than geographic designation. Third, common mutations were observed significantly less frequently in eBL tumors harboring EBV type 1, with mutation frequencies similar between tumors with EBV type 2 and without EBV. In addition to the previously reported genes, a set of new genes mutated in BL including TFAP4, MSH6, PRRC2C, BCL7A, FOXO1, PLCG2, PRKDC, RAD50, and RPRD2 were identified. Overall, these data establish that EBV, particularly EBV type 1, supports BL oncogenesis alleviating the need for certain driver mutations in the human genome.
机译:伯克特地方性淋巴瘤(eBL)是疟疾流行性赤道非洲地区最常见的儿科癌症,几乎总是含有爱泼斯坦-巴尔病毒(EBV),这与散发性的伯基特淋巴瘤(sBL)在发达国家发病率较低有关。考虑到这些差异以及可变的临床表现和结果,我们试图通过使用与多个sBL肿瘤相比的多个原发性eBL肿瘤的RNA测序(RNAseq)研究转录组来进一步了解发病机理。在eBL肿瘤中,基于以下几个方面发现了最小的表达差异:解剖学表现部位,院内存活率和EBV基因组类型;提示eBL肿瘤是均质的,没有明显的亚型。使用替代变量分析检测到的显着差异是与1型EBV相比,携带2型EBV的eBL肿瘤中免疫蛋白酶体复合物中关键基因(PSMB9 /β1i,PSMB10 /β2i,PSMB8 /β5i和PSME2 /PA28β)的表达显着降低。 。其次,与先前发表的儿科sBL标本相比,大多数表达和途径差异与PTEN / PI3K / mTOR信号传导途径有关,并且与EBV状况密切相关,而不与地理标志密切相关。第三,在携带EBV 1型的eBL肿瘤中,常见突变的发生频率显着降低,具有EBV 2型和无EBV的肿瘤之间的突变频率相似。除先前报道的基因外,还鉴定了一组在BL中突变的新基因,包括TFAP4,MSH6,PRRC2C,BCL7A,FOXO1,PLCG2,PRKDC,RAD50和RPRD2。总体而言,这些数据表明,EBV(尤其是1型EBV)支持BL肿瘤发生,从而减轻了人类基因组中某些驱动突变的需求。

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