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补骨脂素衍生的寡核苷酸甲基膦酸酯交联中靶标结构的作用

Effect of target structure on cross-linking by psoralen-derivatized oligonucleoside methylphosphonates.

作者信息

Kean J M, Miller P S

机构信息

Department of Biochemistry, School of Hygiene and Public Health, Johns Hopkins University, Baltimore, Maryland 21205.

出版信息

Biochemistry. 1994 Aug 9;33(31):9178-86. doi: 10.1021/bi00197a021.

DOI:10.1021/bi00197a021
PMID:7519441
Abstract

A series of psoralen-derivatized oligodeoxyribonucleoside methylphosphonates were examined for their abilities to cross-link to DNA and RNA oligonucleotide targets. These targets were designed to have either a random coil or a hairpin structure in solution. The methylphosphonate oligomers cross-linked with approximately the same rates to the random coil DNA and RNA targets, although the extent of cross-linking to the DNA target was higher than that to the RNA target. For a given methylphosphonate sequence, cross-linking decreased as the temperature increased, and this behavior paralleled the interaction of the oligomer with the target as determined by ultraviolet melting experiments. The oligomers also cross-linked efficiently with the DNA hairpin target, but little or no cross-linking was observed with the RNA hairpin. In the case of these hairpin targets, the extent of cross-linking was dependent upon the location of the oligomer binding site relative to the stem and loop regions of the hairpin. The lack of reactivity with the RNA hairpin may be due to the high stability of the stem of this target versus that in the DNA target and the relatively lower efficiency of binding of the methylphosphonates to RNA versus DNA targets. The sequences of the oligomers are complementary to vesicular stomatitis virus M-protein mRNA. One of the oligomers was tested, and was found to cross-link at 20 degrees C to VSV N-mRNA to approximately the same extent as observed for cross-linking with the random coil RNA target, suggesting that the mRNA binding site for the oligomer most likely is in a somewhat open conformation.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

研究了一系列补骨脂素衍生的寡脱氧核糖核苷甲基膦酸酯与DNA和RNA寡核苷酸靶标的交联能力。这些靶标在溶液中设计成具有无规卷曲或发夹结构。甲基膦酸酯寡聚物与无规卷曲的DNA和RNA靶标的交联速率大致相同,尽管与DNA靶标的交联程度高于与RNA靶标的交联程度。对于给定的甲基膦酸酯序列,交联程度随温度升高而降低,这种行为与通过紫外熔化实验确定的寡聚物与靶标的相互作用相似。寡聚物也能与DNA发夹靶标有效交联,但与RNA发夹几乎没有或没有观察到交联。对于这些发夹靶标,交联程度取决于寡聚物结合位点相对于发夹茎和环区域的位置。与RNA发夹缺乏反应性可能是由于该靶标茎相对于DNA靶标茎的高稳定性以及甲基膦酸酯与RNA靶标结合的效率相对低于与DNA靶标结合的效率。寡聚物的序列与水疱性口炎病毒M蛋白mRNA互补。测试了其中一种寡聚物,发现其在20℃下与VSV N-mRNA的交联程度与与无规卷曲RNA靶标交联时观察到的程度大致相同,这表明该寡聚物的mRNA结合位点很可能处于某种开放构象。(摘要截短于250字)

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