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首页> 外文期刊>Virus Research: An International Journal of Molecular and Cellular Virology >Impact of forced selection of tRNAs on HIV-1 replication and genome stability highlight preferences for selection of certain tRNAs.
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Impact of forced selection of tRNAs on HIV-1 replication and genome stability highlight preferences for selection of certain tRNAs.

机译:强制选择tRNA对HIV-1复制和基因组稳定性的影响突出显示了选择某些tRNA的偏好。

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Human immunodeficiency virus (HIV-1) exclusively selects tRNA(Lys,3) as the primer for initiation of reverse transcription. How and why HIV-1 selects the tRNA is unresolved. To address this issue, we have generated HIV-1 in which the PBS was changed to be complementary to alternative tRNAs. In this study, we report on HIV-1 that have the PBS mutated to be complementary to tRNA(Thr), tRNA(Phe), tRNA(Ser) and tRNA(Tyr). Virus with a PBS complementary to tRNA(Thr) grew slightly slower than the wild type virus and maintained the PBS for an extended culture period before finally reverting back to utilize tRNA(Lys,3). In contrast, viruses with a PBS complementary to tRNA(Phe) or tRNA(Ser) rapidly reverted to utilize tRNA(Lys,3) following limited in vitro replication, while a virus with a PBS complementary to tRNA(Tyr) had severely compromised infectivity and did not productively infect a continuous T cell line (SupT1) or human peripheral blood mononuclear cells (PBMC). Modification of the A-loop region to becomplementary to tRNA(Thr) with the mutation in the PBS to be complementary to tRNA(Thr) resulted in a virus that could stably utilize this tRNA while the modification of the A-loop to be complementary to the anticodon of tRNA(Ser) did not allow the virus to stably utilize tRNA(Ser). Modification of the A-loop region to be complementary to the anticodon of tRNA(Phe) severely impacted the replication of this virus. Finally, the modification of the A-loop region to be complementary to tRNA(Tyr) did not rescue the virus with a PBS complementary to tRNA(Tyr). The results of these studies demonstrate the diverse effects that alteration of the PBS to force selection of alternative primers have on HIV-1 replication and provide a framework to understand the dynamics of primer selection.
机译:人类免疫缺陷病毒(HIV-1)仅选择tRNA(Lys,3)作为引发反转录的引物。 HIV-1选择tRNA的方式和原因尚未解决。为了解决这个问题,我们产生了HIV-1,其中PBS被更改为与其他tRNA互补。在这项研究中,我们报道了HIV-1,其PBS突变为与tRNA(Thr),tRNA(Phe),tRNA(Ser)和tRNA(Tyr)互补。含有与tRNA(Thr)互补的PBS的病毒比野生型病毒的生长速度稍慢,并且在延长培养期之前将PBS维持,然后最终恢复使用tRNA(Lys,3)。相反,在有限的体外复制后,具有与tRNA(Phe)或tRNA(Ser)互补的PBS的病毒迅速恢复利用tRNA(Lys,3),而与tRNA(Tyr)互补的PBS的病毒具有严重的传染性。并且没有有效感染连续T细胞系(SupT1)或人外周血单个核细胞(PBMC)。将PBS中的突变与tRNA(Thr)互补,将A环区域修饰为与tRNA(Thr)互补,从而导致病毒可以稳定利用该tRNA,而对A环进行修饰以与tRNA(Thr)互补tRNA(Ser)的反密码子不允许病毒稳定地利用tRNA(Ser)。 A环区域的修饰与tRNA(Phe)的反密码子互补,严重影响了该病毒的复制。最后,将A环区域修饰为与tRNA(Tyr)互补不能用与tRNA(Tyr)互补的PBS拯救病毒。这些研究的结果表明,改变PBS迫使选择其他引物对HIV-1复制具有多种作用,并为理解引物选择的动力学提供了框架。

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