首页> 外文期刊>Bioorganic and Medicinal Chemistry Letters >Complexation of single strand telomere and telomerase RNA template polyanions by deoxyribonucleic guanidine (DNG) polycations: plausible anticancer agents.
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Complexation of single strand telomere and telomerase RNA template polyanions by deoxyribonucleic guanidine (DNG) polycations: plausible anticancer agents.

机译:单链端粒和端粒酶RNA模板聚阴离子通过脱氧核糖核酸胍(DNG)聚阳离子的络合:可能的抗癌剂。

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摘要

Cancerous cell immortality is due to relatively high concentrations of telomerase enzyme which maintains telomere sequence during cell division. Deoxyribonucleic guanidine (DNG) is a positively charged DNA analog in which guanidine replaces the phosphordiester linkage of DNA. Mixed sequences of DNG and DNA oligonucleotides are referred to as chimera. Complexation of DNG and chimeric polycations with the complementary negatively charged non-coding telomere single strand d(5'-TTAGGG-3')(n) and the 11-base telomeric RNA template (5'-CUAACCCUAAC-3') in the active site of telomerase has been studied. Calculated by ensemble sampling simulations in GBMV solvent model, we found that binding of complementary DNG hexamer with telomere is favored over that of DNA-telomere by approximately 10(6)-fold and binding of chimera hexamer is favored by approximately 10(4)-fold. Binding of complementary DNG with telomeric RNA is favored by 43 kcal/mol over telomere substrate binding with telomeric RNA.
机译:癌细胞的永生性是由于端粒酶浓度较高,端粒酶在细胞分裂过程中保持端粒序列。脱氧核糖核酸胍(DNG)是带正电的DNA类似物,其中胍取代了DNA的磷酸二酯键。 DNG和DNA寡核苷酸的混合序列称为嵌合体。 DNG和嵌合聚阳离子与活性中互补的带负电荷的非编码端粒单链d(5'-TTAGGG-3')(n)和11碱基端粒RNA模板(5'-CUAACCCUAAC-3')的复合已经研究了端粒酶的位点。通过GBMV溶剂模型中的整体采样模拟计算,我们发现互补DNG六聚体与端粒的结合比DNA端粒的结合约受10(6)倍的支持,而嵌合六聚体的结合受约10(4)-的促进-折。互补DNG与端粒RNA的结合比与端粒RNA的端粒底物结合更有利于43kcal / mol。

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