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The A-rich RNA sequences of HIV-1 pol are important for the synthesis of viral cDNA

机译:HIV-1 pol的富含A的RNA序列对于病毒cDNA的合成很重要

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The bias of A-rich codons in HIV-1 pol is thought to be a record of hypermutations in viral genomes that lack biological functions. Bioinformatic analysis predicted that A-rich sequences are generally associated with minimal local RNA structures. Using codon modifications to reduce the amount of A-rich sequences within HIV-1 genomes, we have reduced the flexibility of RNA sequences in pol to analyze the functional significance of these A-rich 'structurally poor' RNA elements in HIV-1 pol. Our data showed that codon modification of HIV-1 sequences led to a suppression of virus infectivity by 5-100-fold, and this defect does not correlate with, viral entry, viral protein expression levels, viral protein profiles or virion packaging of genomic RNA. Codon modification of HIV-1 pol correlated with an enhanced dimer stability of the viral RNA genome, which was associated with a reduction of viral cDNA synthesis both during HIV-1 infection and in a cell free reverse transcription assay. Our data provided direct evidence that the HIV-1 A-rich pol sequence is not merely an evolutionary artifact of enzyme-induced hypermutations, and that HIV-1 has adapted to rely on A-rich RNA sequences to support the synthesis of viral cDNA during reverse transcription, highlighting the utility of using 'structurally poor' RNA domains in regulating biological process.
机译:HIV-1 pol中富A密码子的偏倚被认为是缺乏生物学功能的病毒基因组超突变的记录。生物信息学分析预测,富含A的序列通常与最小的局部RNA结构有关。使用密码子修饰来减少HIV-1基因组内HIV丰富的A序列的数量,我们已经降低了pol中RNA序列的灵活性,以分析HIV-1 pol中这些富含A的“结构较差” RNA元素的功能意义。我们的数据表明,HIV-1序列的密码子修饰导致病毒感染性抑制了5-100倍,并且该缺陷与病毒进入,病毒蛋白表达水平,病毒蛋白谱或基因组RNA的病毒粒子包装无关。 HIV-1 pol的密码子修饰与病毒RNA基因组的增强的二聚体稳定性有关,这与在HIV-1感染期间和无细胞逆转录测定中病毒cDNA合成的减少有关。我们的数据提供了直接的证据,表明富含HIV-1 A的pol序列不仅是酶诱导的超突变的进化产物,而且HIV-1已适应于依靠富含A的RNA序列来支持病毒cDNA的合成。反转录,突出了在调控生物过程中使用“结构不良” RNA结构域的实用性。

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