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首页> 外文期刊>Nucleic acids research >Premature strand transfer by the HIV-1 reverse transcriptase during strong-stop DNA synthesis
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Premature strand transfer by the HIV-1 reverse transcriptase during strong-stop DNA synthesis

机译:HIV-1逆转录酶在强终止DNA合成过程中过早转移链

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Reverse transcription of retrovlral genomes starts near the 5′ end of the viral RNA by use of an associated tRNA primer. According to the current model of reverse transcription, the Initial cDNA product, termed minus-strand strong-stop DNA, ‘jumps' to a repeated sequence (R region) at the 3′ end of the RNA template. The human retrovlruses have relatively long R regions (97–247 nucleotides) when compared to murine and avian viruses (16–68 nucleotides). This suggests that the full complement of the R region Is not required for strand transfer and that partial cDNA copies of the 5′ R can prematurely jump to the 3′ R. To test this hypothesis, we generated mutants of the human Immunodeficiency virus with R region changes and analyzed whether 5′ or 3′ R sequences were Inherited by the progeny. We found that In most cases, 5′ R-encoded sequences are dominant, which Is consistent with the model of reverse transcription. Using a selection protocol, however, we were also able to identify progeny viruses with R sequences derived from the original 3′ R element. These results suggest that partial strong stop cDNAs can be transferred with R region homologles much shorter than 97 nucleotides.
机译:逆转录病毒基因组的逆转录通过使用相关的tRNA引物在病毒RNA的5'末端附近开始。根据当前的逆转录模型,称为负链强终止DNA的初始cDNA产物“跳”至RNA模板3'端的重复序列(R区)。与鼠和禽病毒(16-68个核苷酸)相比,人类逆转录病毒具有相对较长的R区(97-247个核苷酸)。这表明链转移不需要R区的完整互补物,而5'R的部分cDNA拷贝可以过早地跳到3'R。为验证这一假设,我们用R生成了人类免疫缺陷病毒的突变体区域变化并分析后代是否继承了5'或3'R序列。我们发现在大多数情况下,5'R编码序列占主导地位,这与反转录模型是一致的。然而,使用选择方案,我们还能够鉴定具有衍生自原始3'R元件的R序列的子代病毒。这些结果表明,可以用短于97个核苷酸的R区同源物转移部分强终止cDNA。

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