与HIV前病毒DNA多嘌呤道形成三螺旋的扭曲嵌入核酸(TINA)序列的优化。

Alexandre S Boutorine, Osman Doluca, Vyacheslav V Filichev
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引用次数: 7

摘要

扭曲的插入核酸与双链DNA的多嘌呤束形成稳定的三联体。它们的亲和力取决于它们的长度、一级结构和碱基含量、寡核苷酸与DNA的平行或反平行取向、TINA残基的数量及其相对位置。基于平行CT、GT和反平行GT三联体形成的靶向HIV前病毒DNA多嘌呤道的16聚寡核苷酸,我们合成了11种不同的寡核苷酸,在不同位置插入2-4个TINA。通过凝胶位移、荧光光谱、圆二色性和热变性等方法研究了它们与靶双聚体的相互作用,结果表明,反平行的GT寡核苷酸比平行的TC或TG寡核苷酸形成更稳定的三聚体。选出两名最优秀的候选人继续深造。第一个(5'-AGGGxGGGTTTxTGTTTT-3', Kd = 219 nM)只包含两个TINA插入,并且在非变性条件下不聚集,这与大多数其他寡核苷酸不同。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Optimization of the sequence of twisted intercalating nucleic acids (TINA) forming triple helix with the polypurine tract of the proviral HIV DNA.

Twisted intercalating nucleic acids form stable triplexes with polypurine tracts of double-stranded DNA. Their affinity depends on their length, primary structure and base contents, parallel or antiparallel orientation of oligonucleotides respectively to DNA, number of TINA residues and their relative positions. Basing on parallel CT, GT and antiparallel GT triplex-forming 16-mer oligonucleotides targeted to polypurine tract of HIV proviral DNA, we synthesized eleven different oligonucleotides with 2-4 TINA insertions in different positions. Studies of their interaction with target duplex by gel shift, fluorescence spectroscopy, circular dichroism and thermal denaturation demonstrated that antiparallel GT oligonucleotides form more stable triplexes than parallel TC or TG ones. Two best candidates were selected for the further studies. The first one (5'-AGGGxGGGTTTxTGTTTT-3', Kd = 219 nM) contains only two TINA insertions and does not aggregate in non-denaturing conditions, in contrast to majority of other oligonucleotides.

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