含有甲基膦酸键的发夹寡核苷酸与HIV TAR RNA的相互作用。

Tomoko Hamma, Paul S Miller
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引用次数: 9

摘要

制备了长度为15 ~ 20个核苷酸(nt)的甲基膦酸修饰寡聚-2′- o-甲基核糖核苷酸,其序列与HIV反式反应元件(TAR) RNA上发夹的5′和3′侧互补。这些抗TAR寡核苷酸(odn)形成稳定的发夹,其熔化温度(Tm)在55℃至80℃之间。尽管它们具有相当高的热稳定性,但发夹寡核苷酸-2'- o-甲基核糖核苷酸与TAR RNA形成非常稳定的配合物,在37℃时解离常数在纳摩尔浓度范围内。由于在该低聚物的TAR环互补区(TLCR)存在两个甲基膦酸键,结合亲和力降低了约17倍,而该区域外的甲基膦酸键使结合亲和力提高了约3倍。TLCR中甲基膦酸盐键的构型也会影响其结合亲和力,其中RpRp异构体的结合明显高于SpSp异构体。除了作为低聚物与TAR RNA相互作用的探针外,甲基膦酸键与发夹结构结合的存在增加了这些低聚物对哺乳动物血清中发现的外切酶降解的抵抗力。含有甲基膦酸盐键的发夹odn具有高结合亲和力和核酸酶抗性,这表明它们具有作为反义化合物的潜在用途。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Interactions of hairpin oligo-2'-O-methylribonucleotides containing methylphosphonate linkages with HIV TAR RNA.

Methylphosphonate-modified oligo-2'-O-methylribonucleotides 15-20 nucleotides (nt) in length were prepared whose sequences are complementary to the 5' and 3' sides of the upper hairpin of HIV trans-acting response element (TAR) RNA. These anti-TAR oligonucleotides (ODNs) form stable hairpins whose melting temperatures (Tm) range from 55 degrees C to 80 degrees C. Despite their rather high thermal stabilities, the hairpin oligo-2'-O-methylribonucleotides formed very stable complexes with TAR RNA, with dissociation constants in the nanomolar concentration range at 37 degrees C. The affinities of the hairpin oligomers for TAR RNA were influenced by the positions of the methylphosphonate linkages. The binding affinity was reduced approximately 17-fold by the presence of two methylphosphonate linkages in the TAR loop complementary region (TLCR) of the oligomer, whereas methylphosphonate linkages outside this region increased binding affinity approximately 3-fold. The configurations of the methylphosphonate linkages in the TLCR also affected binding affinity, with the RpRp isomer showing significantly higher binding than the SpSp isomer. In addition to serving as probes of the interactions between the oligomer and TAR RNA, the presence of the methylphosphonate linkages in combination with the hairpin structure increases the resistance of these oligomers to degradation by exonucleases found in mammalian serum. The combination of high binding affinity and nuclease resistance of the hairpin ODNs containing methylphosphonate linkages suggests their potential utility as antisense compounds.

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