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γ逆转录病毒中的反义转录作为一种插入激活宿主基因的机制。

Antisense transcription in gammaretroviruses as a mechanism of insertional activation of host genes.

机构信息

Department of Molecular Biology, C.F. Møllers Allé 3, 1.130, Aarhus University, DK-8000 Arhus C, Denmark.

出版信息

J Virol. 2010 Apr;84(8):3780-8. doi: 10.1128/JVI.02088-09. Epub 2010 Feb 3.

Abstract

Transcription of retroviruses is initiated at the U3-R region boundary in the integrated provirus and continues unidirectionally to produce genomic and mRNA products of positive polarity. Several studies have recently demonstrated the existence of naturally occurring protein-encoding transcripts of negative polarity in complex retroviruses. We report here on the identification of transcripts of negative polarity in simple murine leukemia virus (MLV). In T-cell and B-cell lymphomas induced by SL3-3 and Akv MLV, antisense transcripts initiated in the U3 region of the proviral 5' long terminal repeat (LTR) and continued into the cellular proto-oncogenes Jdp2 and Bach2 to create chimeric transcripts consisting of viral and host sequence. The phenomenon was validated in vivo using a knock-in mouse model homozygous for a single LTR at a position known to activate Nras in B-cell lymphomas. A 5' rapid amplification of cDNA ends (RACE) analysis indicated a broad spectrum of initiation sites within the U3 region of the 5' LTR. Our data show for the first time transcriptional activity of negative polarity initiating in the U3 region of simple retroviruses and suggest a novel mechanism of insertional activation of host genes. Elucidation of the nature and potential regulatory role of 5' LTR antisense transcription will be relevant to the design of therapeutic vectors and may contribute to the increasing recognition of pervasive eukaryotic transcription.

摘要

逆转录病毒的转录起始于整合前病毒的 U3-R 区域边界,并单向进行,产生正链基因组和 mRNA 产物。最近的几项研究表明,复杂逆转录病毒中存在自然发生的负链蛋白编码转录本。我们在此报告在简单鼠白血病病毒(MLV)中鉴定到负链转录本。在 SL3-3 和 Akv MLV 诱导的 T 细胞和 B 细胞淋巴瘤中,反义转录本起始于前病毒 5'长末端重复(LTR)的 U3 区,并延伸到细胞原癌基因 Jdp2 和 Bach2 中,产生包含病毒和宿主序列的嵌合转录本。该现象在体内使用一个在已知会激活 B 细胞淋巴瘤中 Nras 的位置上纯合单个 LTR 的敲入小鼠模型得到了验证。5' 快速扩增 cDNA 末端(RACE)分析表明,5'LTR 的 U3 区内存在广泛的起始位点。我们的数据首次显示了简单逆转录病毒 U3 区内负链转录的转录活性,并提出了一种宿主基因插入激活的新机制。阐明 5'LTR 反义转录的性质和潜在调控作用,将与治疗性载体的设计相关,并可能有助于日益认识到普遍存在的真核转录。

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