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FLI1 是一种新型 ETS 转录因子,参与前列腺癌中的基因融合。

FLI1 is a novel ETS transcription factor involved in gene fusions in prostate cancer.

机构信息

Department of Genetics, Portuguese Oncology Institute, Porto, Portugal.

出版信息

Genes Chromosomes Cancer. 2012 Mar;51(3):240-9. doi: 10.1002/gcc.20948. Epub 2011 Nov 12.

Abstract

To characterize the pattern of ETS rearrangements and to uncover novel ETS fusion genes, we analyzed 200 prostate carcinomas (PCa) with TaqMan low-density arrays (TLDAs), followed by selective analyses with fluorescence in situ hybridization (FISH), RT-PCR, and sequencing. Besides confirming the recurrent presence of ERG, ETV1, ETV4, and ETV5 rearrangements, we here report FLI1 as the fifth ETS transcription factor involved in fusion genes in prostate cancer. Outlier expression of the FLI1 gene was detected by TLDAs in one PCa that showed relative overexpression of FLI1 exons 4:5 as compared with FLI1 exons 2:3. A structural rearrangement was found using FISH probes flanking the FLI1 gene and RT-PCR and sequencing analyses showed fusion of SLC45A3 exon 1 with FLI1 exon 3. Interestingly, we found four cases with two different ETS rearrangements in the index tumor, thus revealing intratumor genetic heterogeneity. Correlation analysis with clinico-pathological data showed association of ERG rearrangements with locally advanced disease (pT3, P = 0.007) and MYC overexpression (P = 0.001), and association of ETV1 rearrangements with PTEN downregulation (P = 0.015). We report that FLI1 is a novel ETS transcription factor involved in gene fusions in prostate cancer and that intratumor genetic heterogeneity of ETS rearrangements can occasionally be found in index primary tumors.

摘要

为了描述 ETS 重排的模式并揭示新的 ETS 融合基因,我们使用 TaqMan 低密度阵列(TLDAs)分析了 200 例前列腺癌(PCa),随后通过荧光原位杂交(FISH)、RT-PCR 和测序进行了选择性分析。除了确认 ERG、ETV1、ETV4 和 ETV5 重排的反复出现外,我们还报告了 FLI1 作为第五个参与前列腺癌融合基因的 ETS 转录因子。TLDAs 检测到一个 PCa 中 FLI1 基因的异常表达,该 PCa 中 FLI1 外显子 4:5 的相对过表达与 FLI1 外显子 2:3 相比。使用侧翼 FLI1 基因的 FISH 探针发现了结构重排,RT-PCR 和测序分析显示 SLC45A3 外显子 1 与 FLI1 外显子 3 融合。有趣的是,我们发现四个病例在索引肿瘤中存在两种不同的 ETS 重排,从而揭示了肿瘤内遗传异质性。与临床病理数据的相关性分析显示,ERG 重排与局部进展性疾病(pT3,P = 0.007)和 MYC 过表达(P = 0.001)相关,而 ETV1 重排与 PTEN 下调相关(P = 0.015)。我们报告称,FLI1 是一种新的 ETS 转录因子,参与前列腺癌中的基因融合,并且在索引原发性肿瘤中偶尔可以发现 ETS 重排的肿瘤内遗传异质性。

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