Briggs Erica M, McKerrow Wilson, Mita Paolo, Boeke Jef D, Logan Susan K, Fenyö David
Departments of Biochemistry and Molecular Pharmacology, New York University, 450 East 29th Street, Room 321, New York, NY, 10016, USA.
Institute for Systems Genetics, New York University Grossman School of Medicine, 435 East 30th St, 9th Floor, NY, 10016, New York, USA.
Mob DNA. 2021 Feb 9;12(1):5. doi: 10.1186/s13100-021-00233-3.
Long INterspersed Element-1 (LINE-1) is an autonomous retroelement able to "copy-and-paste" itself into new loci of the host genome through a process called retrotransposition. The LINE-1 bicistronic mRNA codes for two proteins, ORF1p, a nucleic acid chaperone, and ORF2p, a protein with endonuclease and reverse transcriptase activity. Both proteins bind LINE-1 mRNA in cis and are necessary for retrotransposition. While LINE-1 transcription is usually repressed in most healthy somatic cells through a plethora of mechanisms, ORF1p expression has been observed in nearly 50% of tumors, and new LINE-1 insertions have been documented in a similar fraction of tumors, including prostate cancer.
Here, we utilized RNA ImmunoPrecipitation (RIP) and the L1EM analysis software to identify ORF1p bound RNA in prostate cancer cells. We identified LINE-1 loci that were expressed in parental androgen sensitive and androgen independent clonal derivatives. In all androgen independent cells, we found higher levels of LINE-1 RNA, as well as unique expression patterns of LINE-1 loci. Interestingly, we observed that ORF1p bound many non-LINE-1 mRNA in all prostate cancer cell lines evaluated, and polyA RNA, and RNA localized in p-bodies were especially enriched. Furthermore, the expression levels of RNAs identified in our ORF1p RIP correlated with RNAs expressed in LINE-1 positive tumors from The Cancer Genome Atlas (TCGA).
Our results show a significant remodeling of LINE-1 loci expression in androgen independent cell lines when compared to parental androgen dependent cells. Additionally, we found that ORF1p bound a significant amount of non-LINE-1 mRNA, and that the enriched ORF1p bound mRNAs are also amplified in LINE-1 expressing TCGA prostate tumors, indicating the biological relevance of our findings to prostate cancer.
长散在核元件1(LINE-1)是一种自主反转录元件,能够通过一种称为反转录转座的过程将自身“复制并粘贴”到宿主基因组的新位点。LINE-1双顺反子mRNA编码两种蛋白质,即核酸伴侣ORF1p和具有内切核酸酶及逆转录酶活性的ORF2p。这两种蛋白质均以顺式结合LINE-1 mRNA,并且是反转录转座所必需的。虽然在大多数健康体细胞中,LINE-1转录通常通过多种机制受到抑制,但在近50%的肿瘤中观察到了ORF1p的表达,并且在类似比例的肿瘤(包括前列腺癌)中记录到了新的LINE-1插入。
在这里,我们利用RNA免疫沉淀(RIP)和L1EM分析软件来鉴定前列腺癌细胞中与ORF1p结合的RNA。我们鉴定出了在亲本雄激素敏感和雄激素非依赖性克隆衍生物中表达的LINE-1位点。在所有雄激素非依赖性细胞中,我们发现LINE-1 RNA水平更高,以及LINE-1位点的独特表达模式。有趣的是,我们观察到在所有评估的前列腺癌细胞系中,ORF1p结合了许多非LINE-1 mRNA、多聚腺苷酸RNA,并且定位于P小体的RNA尤其富集。此外,我们在ORF1p RIP中鉴定出的RNA表达水平与来自癌症基因组图谱(TCGA)的LINE-1阳性肿瘤中表达的RNA相关。
我们的结果表明,与亲本雄激素依赖性细胞相比,雄激素非依赖性细胞系中LINE-1位点的表达发生了显著重塑。此外,我们发现ORF1p结合了大量非LINE-1 mRNA,并且在表达LINE-1的TCGA前列腺肿瘤中,富集的与ORF1p结合的mRNA也被扩增,这表明我们的发现与前列腺癌具有生物学相关性。
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