首页> 美国卫生研究院文献>Nucleic Acids Research >Anomeric inversion (from beta to alpha) in methylphosphonate oligonucleosides enhances their affinity for DNA and RNA.
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Anomeric inversion (from beta to alpha) in methylphosphonate oligonucleosides enhances their affinity for DNA and RNA.

机译:甲基膦酸寡核苷酸中的端基转化(从β到α)增加了它们对DNA和RNA的亲和力。

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摘要

Here we report that the poor binding of methylphosphonate oligodeoxynucleosides (MP-ODNs) to their nucleic acid targets can be improved by additional inversion of the anomeric configuration (from beta to alpha) in the sugar moieties to give a new class of analogs, MP alpha-oligonucleosides. MP alpha-dT12and MP 5' alpha-d(TCTTAACCCACA) 3' were synthesized and their ability to form hybrids with complementary single stranded (ss)DNA and ssRNA, as well as with double stranded (ds)DNA, was evaluated. The thermal stability of hybrids formed with MP alpha-analogs was compared with the affinity of phosphodiester (PO) and phosphorothioate (PS) beta- and alpha-oligomers for their targets. Non-ionic MP alpha-oligonucleosides bound to their complementary DNA and RNA strands more tightly than their homologues with natural beta-anomeric configuration did. With DNA target, MP alpha-oligomers formed duplexes more stable than the corresponding natural PO beta-oligomer did. MP alpha-heteropolymer hybridized to RNA target better than PS beta-oligonucleotide did but the hybrid was less stable (DeltaTm-0.5 degrees C per mod.) than the hybrid formed with the natural PO beta-oligomer. Only MP alpha-dT12 bound to dsDNA target at low salt concentration (0.1 M NaCl).
机译:在这里我们报告说,可以通过糖部分的异头构型(从β到α)的额外转化来改善甲基膦酸寡聚脱氧核苷(MP-ODN)与其核酸靶标的结合不良,从而产生一类新的类似物,MPα -寡核苷。合成了MP alpha-dT12和MP 5'alpha-d(TCTTAACCCACA)3',并评估了它们与互补单链(ss)DNA和ssRNA以及双链(ds)DNA形成杂种的能力。将与MPα-类似物形成的杂化物的热稳定性与磷酸二酯(PO)和硫代磷酸酯(PS)β-和α-低聚物对其靶标的亲和力进行了比较。非离子MPα-寡核苷与其互补的DNA和RNA链的结合要比其具有天然β-异头异构体配置的同系物更紧密。使用DNA靶标,MPα-低聚物形成的双链体比相应的天然POβ-低聚物更稳定。与PSβ-寡核苷酸相比,与RNA靶杂交的MPα-杂聚物比与天然POβ-寡聚体形成的杂合体更不稳定(DeltaTm-0.5°C / mod。)。只有MP alpha-dT12在低盐浓度(0.1 M NaCl)下与dsDNA结合。

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