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首页> 外文期刊>Nucleic acids research >Duplex structural differences and not 2′-hydroxyls explain the more stable binding of HIV-reverse transcriptase to RNA-DNA versus DNA-DNA
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Duplex structural differences and not 2′-hydroxyls explain the more stable binding of HIV-reverse transcriptase to RNA-DNA versus DNA-DNA

机译:双链体结构差异而非2'-羟基解释了HIV逆转录酶与RNA-DNA相比DNA-DNA更稳定的结合

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摘要

Human immunodeficiency virus reverse transcriptase (HIV-RT) binds more stably in binary complexes with RNA–DNA versus DNA–DNA. Current results indicate that only the -2 and -4 RNA nucleotides (-1 hybridized to the 3′ recessed DNA base) are required for stable binding to RNA–DNA, and even a single RNA nucleotide conferred significantly greater stability than DNA–DNA. Replacing 2′- hydroxyls on pivotal RNA bases with 2′-O-methyls did not affect stability, indicating that interactions between hydroxyls and RT amino acids do not stabilize binding. RT's Kd (koff/kon) for DNA–DNA and RNA–DNA were similar, although koff differed almost 40-fold, suggesting a faster kon for DNA–DNA. Avian myeloblastosis and Moloney murine leukemia virus RTs also bound more stably to RNA–DNA, but the difference was less pronounced than with HIV-RT. We propose that the H- versus B-form structures of RNA–DNA and DNA–DNA, respectively, allow the former to conform more easily to HIV-RT's binding cleft, leading to more stable binding. Biologically, the ability of RT to form a more stable complex on RNA–DNA may aid in degradation of RNA fragments that remain after DNA synthesis.
机译:人类免疫缺陷病毒逆转录酶(HIV-RT)与RNA-DNA和DNA-DNA的二元复合体结合更稳定。目前的结果表明,仅需-2和-4 RNA核苷酸(-1与3'凹陷的DNA碱基杂交)即可稳定地与RNA-DNA结合,甚至单个RNA核苷酸也比DNA-DNA具有更大的稳定性。用2'-O-甲基取代关键RNA碱基上的2'-羟基不会影响稳定性,表明羟基与RT氨基酸之间的相互作用无法稳定结合。 RT的DNA–DNA和RNA–DNA的K d (k off / k on )相似,尽管k off 相差近40倍,表明DNA–DNA的k on 更快。禽成纤维细胞病和莫洛尼鼠白血病病毒RTs也更稳定地与RNA-DNA结合,但这种差异不如HIV-RT明显。我们提出,RNA–DNA和DNA–DNA的H型和B型结构分别使前者更容易适应HIV-RT的结合裂隙,从而导致更稳定的结合。从生物学上讲,RT在RNA-DNA上形成更稳定的复合物的能力可能有助于降解DNA合成后残留的RNA片段。

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