Elfman Justin, Goins Lynette, Heller Tessa, Singh Sandeep, Wang Yuh-Hwa, Li Hui
bioRxiv. 2023 Feb 3:2023.02.02.526864. doi: 10.1101/2023.02.02.526864.
Gene fusions and their chimeric products are typically considered hallmarks of cancer. However, recent studies have found chimeric transcripts in non-cancer tissues and cell lines. In addition, efforts to annotate structural variation at large scale have found examples of gene fusions with potential to produce chimeric transcripts in normal tissues. In this report, we provide a means for targeting population-specific chimeric RNAs to enrich for those generated by gene fusion events. We identify 57 such chimeric RNAs from the GTEx cohort, including , whose distribution we assessed across the populations of the 1000 Genomes Project. We reveal that results from a common complex structural variant in populations with African heritage, and identify its likely mechanism for formation. Additionally, we utilize a large cohort of clinical samples to characterize the chimeric RNA, and find an association between the variant and indications of Neurofibramatosis Type I. We present this gene fusion as a case study for identifying hard-to-find and potentially functional structural variants by selecting for those which produce population-specific fusion transcripts.
基因融合及其嵌合产物通常被视为癌症的标志。然而,最近的研究在非癌组织和细胞系中发现了嵌合转录本。此外,大规模注释结构变异的研究发现了一些基因融合的例子,这些基因融合有可能在正常组织中产生嵌合转录本。在本报告中,我们提供了一种靶向群体特异性嵌合RNA的方法,以富集那些由基因融合事件产生的嵌合RNA。我们从GTEx队列中鉴定出57种这样的嵌合RNA,包括 ,我们评估了其在千人基因组计划各群体中的分布。我们发现 是非洲裔群体中一种常见的复杂结构变异的结果,并确定了其可能的形成机制。此外,我们利用大量临床样本对 嵌合RNA进行表征,发现该变异与I型神经纤维瘤病的指征之间存在关联。我们将这种基因融合作为一个案例研究,通过选择那些产生群体特异性融合转录本的变异来识别难以发现的潜在功能性结构变异。
——发现57种多态性嵌合RNA——表征SUZ12P1-CRLF3多态性嵌合RNA及相应重排——识别产生转录基因融合的结构变异的新型自下而上方法。
