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鼠白血病病毒R区域的二级结构对于刺激长末端重复序列驱动的基因表达很重要。

The secondary structure of the R region of a murine leukemia virus is important for stimulation of long terminal repeat-driven gene expression.

作者信息

Cupelli L, Okenquist S A, Trubetskoy A, Lenz J

机构信息

Department of Molecular Genetics, Albert Einstein College of Medicine, Bronx, New York 10461, USA.

出版信息

J Virol. 1998 Oct;72(10):7807-14. doi: 10.1128/JVI.72.10.7807-7814.1998.

Abstract

In addition to their role in reverse transcription, the R-region sequences of some retroviruses affect viral transcription. The first 28 nucleotides of the R region within the long terminal repeat (LTR) of the murine type C retrovirus SL3 were predicted to form a stem-loop structure. We tested whether this structure affected the transcriptional activity of the viral LTR. Mutations that altered either side of the stem and thus disrupted base pairing were generated. These decreased the level of expression of a reporter gene under the control of viral LTR sequences about 5-fold in transient expression assays and 10-fold in cells stably transformed with the LTR-reporter plasmids. We also generated a compensatory mutant in which both the ascending and descending sides of the stem were mutated such that the nucleotide sequence was different but the predicted secondary structure was maintained. Most of the activity of the wild-type SL3 element was restored in this mutant. Thus, the stem-loop structure was important for the maximum activity of the SL3 LTR. Primer extension analysis indicated that the stem-loop structure affected the levels of cytoplasmic RNA. Nuclear run-on assays indicated that deletion of the R region had a small effect on transcriptional initiation and no effect on RNA polymerase processivity. Thus, the main effect of the R-region element was on one or more steps that occurred after the template was transcribed by RNA polymerase. This finding implied that the main function of the R-region element involved RNA processing. R-region sequences of human immunodeficiency virus type 1 or mouse mammary tumor virus could not replace the SL3 element. R-region sequences from an avian reticuloendotheliosis virus partially substituted for the SL3 sequences. R-region sequences from Moloney murine leukemia virus or feline leukemia virus did function in place of the SL3 element. Thus, the R region element appears to be a general feature of the mammalian type C genus of retroviruses.

摘要

除了在逆转录过程中的作用外,一些逆转录病毒的R区域序列还会影响病毒转录。鼠类C型逆转录病毒SL3的长末端重复序列(LTR)内R区域的前28个核苷酸预计会形成茎环结构。我们测试了这种结构是否会影响病毒LTR的转录活性。产生了改变茎两侧从而破坏碱基配对的突变。在瞬时表达试验中,这些突变使病毒LTR序列控制下的报告基因表达水平降低了约5倍,在用LTR-报告质粒稳定转化的细胞中降低了10倍。我们还产生了一个补偿性突变体,其中茎的上升和下降两侧都发生了突变,使得核苷酸序列不同但预测的二级结构得以维持。在这个突变体中,野生型SL3元件的大部分活性得以恢复。因此,茎环结构对于SL3 LTR的最大活性很重要。引物延伸分析表明,茎环结构影响细胞质RNA的水平。细胞核连续转录分析表明,R区域的缺失对转录起始有较小影响,对RNA聚合酶的持续合成能力没有影响。因此,R区域元件的主要作用是在RNA聚合酶转录模板之后发生的一个或多个步骤上。这一发现表明,R区域元件的主要功能涉及RNA加工。1型人类免疫缺陷病毒或小鼠乳腺肿瘤病毒的R区域序列不能替代SL3元件。禽网状内皮组织增生症病毒的R区域序列部分替代了SL3序列。莫洛尼鼠白血病病毒或猫白血病病毒的R区域序列确实能替代SL3元件发挥作用。因此,R区域元件似乎是逆转录病毒哺乳动物C型属的一个普遍特征。

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