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一种人类内源性逆转录病毒HERV-H与两个相邻人类基因之间的基因间剪接。

Intergenic splicing between a HERV-H endogenous retrovirus and two adjacent human genes.

作者信息

Kowalski P E, Freeman J D, Mager D L

机构信息

Department of Medical Genetics, University of British Columbia, Vancouver, British Columbia, V5Z 1L3, Canada.

出版信息

Genomics. 1999 May 1;57(3):371-9. doi: 10.1006/geno.1999.5787.

Abstract

We previously reported that a long terminal repeat (LTR) of a human endogenous retrovirus of the HERV-H family promotes expression of a cellular fusion transcript in teratocarcinoma cell lines. This transcript was termed PLA2L due to two regions of similarity to the secreted form of phospholipase A2. In this study, evidence is presented indicating that this transcript appears to be the result of intergenic splicing between the HERV-H element and two independent downstream genes. The 5' gene has been named HHLA1 (HERV-H LTR-associating 1) and is of unknown function but shows sequence conservation in other mammals. The 3' gene is now known to encode human otoconin-90 (OC90) which, in mice, is a major protein expressed in the fetal inner ear. Evidence for intergenic splicing of these two genes includes: (1) the isolation of LTR-driven HHLA1 transcripts, unspliced to otoconin-90 exons, with variable sites of polyadenylation; (2) the cloning of both the putative human intergenic genomic region and the novel 5' terminus of the mouse otoconin-90 gene; (3) the identification of homologous potential signal sequences in the 5' region of mouse otoconin-90 and in the middle of the PLA2L transcript; and (4) the lack of detectable chromosomal rearrangements involving this region in teratocarcinoma cells. The PLA2L transcript therefore represents a rare example of intergenic splicing of two closely linked genes. We hypothesize that human HHLA1 and OC90 are normally expressed independently from different promoters but are expressed from the LTR promoter and spliced together in teratocarcinoma cells. It is tempting to speculate that the high activity of the LTR promoter in this cell type may induce transcriptional fusion between these two genes.

摘要

我们之前报道过,人类内源性逆转录病毒HERV-H家族的长末端重复序列(LTR)可促进畸胎瘤细胞系中一种细胞融合转录本的表达。由于该转录本与分泌型磷脂酶A2有两个相似区域,因此被命名为PLA2L。在本研究中,有证据表明该转录本似乎是HERV-H元件与两个独立的下游基因之间基因间剪接的结果。5'端基因已被命名为HHLA1(HERV-H LTR关联基因1),功能未知,但在其他哺乳动物中显示出序列保守性。现在已知3'端基因编码人类耳石素-90(OC90),在小鼠中,它是胎儿内耳中表达的主要蛋白质。这两个基因发生基因间剪接的证据包括:(1)分离出由LTR驱动的、未剪接到耳石素-90外显子的HHLA1转录本,其具有可变的聚腺苷酸化位点;(2)克隆了推测的人类基因间基因组区域以及小鼠耳石素-90基因的新5'端;(3)在小鼠耳石素-90的5'区域和PLA2L转录本中间鉴定出同源的潜在信号序列;(4)在畸胎瘤细胞中未检测到涉及该区域的染色体重排。因此,PLA2L转录本代表了两个紧密相连基因发生基因间剪接的罕见例子。我们推测,人类HHLA1和OC90通常从不同启动子独立表达,但在畸胎瘤细胞中从LTR启动子表达并剪接在一起。很容易推测,这种细胞类型中LTR启动子的高活性可能诱导了这两个基因之间的转录融合。

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