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室管膜瘤中的新型融合基因和嵌合转录本

Novel fusion genes and chimeric transcripts in ependymal tumors.

作者信息

Olsen Thale Kristin, Panagopoulos Ioannis, Gorunova Ludmila, Micci Francesca, Andersen Kristin, Kilen Andersen Hege, Meling Torstein R, Due-Tønnessen Bernt, Scheie David, Heim Sverre, Brandal Petter

机构信息

Section for Cancer Cytogenetics, Institute for Cancer Genetics and Informatics, Oslo University Hospital, Norway.

Centre for Cancer Biomedicine, Faculty of Medicine, University of Oslo, Norway.

出版信息

Genes Chromosomes Cancer. 2016 Dec;55(12):944-953. doi: 10.1002/gcc.22392. Epub 2016 Jul 28.

Abstract

We have previously identified two ALK rearrangements in a subset of ependymal tumors using a combination of cytogenetic data and RNA sequencing. The aim of this study was to perform an unbiased search for fusion transcripts in our entire series of ependymal tumors. Fusion analysis was performed using the FusionCatcher algorithm on 12 RNA-sequenced ependymal tumors. Candidate transcripts were prioritized based on the software's filtering and manual visualization using the BLAST (Basic Local Alignment Search Tool) and BLAT (BLAST-like alignment tool) tools. Genomic and reverse transcriptase PCR with subsequent Sanger sequencing was used to validate the potential fusions. Fluorescent in situ hybridization (FISH) using locus-specific probes was also performed. A total of 841 candidate chimeric transcripts were identified in the 12 tumors, with an average of 49 unique candidate fusions per tumor. After algorithmic and manual filtering, the final list consisted of 24 potential fusion events. Raw RNA-seq read sequences and PCR validation supports two novel fusion genes: a reciprocal fusion gene involving UQCR10 and C1orf194 in an adult spinal ependymoma and a TSPAN4-CD151 fusion gene in a pediatric infratentorial anaplastic ependymoma. Our previously reported ALK rearrangements and the RELA and YAP1 fusions found in supratentorial ependymomas were until now the only known fusion genes present in ependymal tumors. The chimeric transcripts presented here are the first to be reported in infratentorial or spinal ependymomas. Further studies are required to characterize the genomic rearrangements causing these fusion genes, as well as the frequency and functional importance of the fusions. © 2016 Wiley Periodicals, Inc.

摘要

我们之前通过细胞遗传学数据和RNA测序相结合的方法,在一部分室管膜瘤中鉴定出两种ALK重排。本研究的目的是在我们的整个室管膜瘤系列中进行无偏倚的融合转录本搜索。使用FusionCatcher算法对12个RNA测序的室管膜瘤进行融合分析。候选转录本根据软件的筛选以及使用BLAST(基本局部比对搜索工具)和BLAT(类BLAST比对工具)工具的手动可视化进行优先级排序。采用基因组和逆转录酶PCR以及随后的Sanger测序来验证潜在的融合。还使用位点特异性探针进行了荧光原位杂交(FISH)。在这12个肿瘤中共鉴定出841个候选嵌合转录本,每个肿瘤平均有49个独特的候选融合。经过算法和手动筛选后,最终列表包含24个潜在的融合事件。原始RNA-seq读取序列和PCR验证支持两个新的融合基因:一个在成人脊髓室管膜瘤中涉及UQCR10和C1orf194的相互融合基因,以及一个在儿童幕下间变性室管膜瘤中的TSPAN4-CD151融合基因。我们之前报道的ALK重排以及在幕上室管膜瘤中发现的RELA和YAP1融合,到目前为止是室管膜瘤中仅有的已知融合基因。这里呈现的嵌合转录本是首次在幕下或脊髓室管膜瘤中报道。需要进一步研究来表征导致这些融合基因的基因组重排,以及融合的频率和功能重要性。© 2016威利期刊公司

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