首页> 外文期刊>Journal of Medicinal Chemistry >In vitro and in vivo activities of oligodeoxynucleotide-based thrombin inhibitors containing neutral formacetal linkages.
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In vitro and in vivo activities of oligodeoxynucleotide-based thrombin inhibitors containing neutral formacetal linkages.

机译:含中性甲缩醛键的基于寡聚脱氧核苷酸的凝血酶抑制剂的体外和体内活性。

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摘要

A series of 15-mer oligodeoxynucleotide analogues were synthesized, and their thrombin inhibitory activities in vitro and in vivo were evaluated. These oligodeoxynucleotide analogues share the same sequence (GGTTGGTGTGGTTGG) but have one or more phosphodiester linkages replaced by a neutral formacetal group. The results obtained from monosubstitutions show that no single phosphodiester group is critical for the thrombin inhibitory activity, suggesting that the interaction between the oligodeoxynucleotide and thrombin is based on a multiple-site charge-charge interaction. Analysis of the effects of different phosphodiester replacements indicates that the backside and left side of the chairlike structure formed by the molecule may be involved in binding with thrombin, presumably by having direct contacts with the anion-binding exosite of the enzyme. For the oligodeoxynucleotides containing two noncontiguous formacetal groups, the effect of the disubstitution is the sum of the effects obtained from the corresponding two monosubstitutions. Infusion of an oligodeoxynucleotide containing four formacetal groups into monkeys showed an increased in vivo anticoagulant effect and an extended in vivo half-life compared to the unmodified oligodeoxynucleotide.
机译:合成了一系列的15-mer寡脱氧核苷酸类似物,并评估了它们在体外和体内的凝血酶抑制活性。这些寡脱氧核苷酸类似物具有相同的序列(GGTTGGTGTGGTTGG),但是具有一个或多个被中性缩醛基团取代的磷酸二酯键。从单取代获得的结果表明,没有单个磷酸二酯基团对凝血酶抑制活性至关重要,这表明寡脱氧核苷酸与凝血酶之间的相互作用是基于多位电荷-电荷相互作用。对不同磷酸二酯置换作用的分析表明,该分子形成的椅状结构的背面和左侧可能与凝血酶结合,大概是通过与酶的阴离子结合异位点直接接触。对于含有两个不连续的甲缩醛基团的寡脱氧核苷酸,解离作用是从相应的两个单取代获得的作用之和。与未修饰的寡聚脱氧核苷酸相比,向猴子中输注含有四个甲缩醛基团的寡聚脱氧核苷酸显示出增加的体内抗凝作用和延长的体内半衰期。

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