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G-quadruplex induced stabilization by 2′-deoxy-2′-fluoro-d-arabinonucleic acids (2′F-ANA)

机译:G-四链体通过2'-脱氧-2'-氟-d-阿拉伯糖核酸(2'F-ANA)诱导稳定

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摘要

The impact of 2′-deoxy-2′-fluoroarabinonucleotide residues (2′F-araN) on different G-quadruplexes derived from a thrombin-binding DNA aptamer d(G2T2G2TGTG2T2G2), an anti-HIV phosphorothioate aptamer PS-d(T2G4T2) and a DNA telomeric sequence d(G4T4G4) via UV thermal melting (Tm) and circular dichroism (CD) experiments has been investigated. Generally, replacement of deoxyguanosines that adopt the anti conformation (anti-guanines) with 2′F-araG can stabilize G-quartets and maintain the quadruplex conformation, while replacement of syn-guanines with 2′F-araG is not favored and results in a dramatic switch to an alternative quadruplex conformation. It was found that incorporation of 2′F-araG or T residues into a thrombin-binding DNA G-quadruplex stabilizes the complex (ΔTm up to ∼+3°C/2′F-araN modification); 2′F-araN units also increased the half-life in 10% fetal bovine serum (FBS) up to 48-fold. Two modified thrombin-binding aptamers (PG13 and PG14) show an approximately 4-fold increase in binding affinity to thrombin, as assessed via a nitrocellulose filter binding assay, both with increased thermal stability (∼1°C/2′F-ANA modification increase in Tm) and nuclease resistance (4–7-fold) as well. Therefore, the 2′-deoxy-2′-fluoro-d-arabinonucleic acid (2′F-ANA) modification is well suited to tune (and improve) the physicochemical and biological properties of naturally occurring DNA G-quartets.
机译:2'-脱氧-2'-氟阿拉伯糖核苷酸残基(2'F-araN)对衍生自凝血酶结合DNA适体d(G2T2G2TGTG2T2G2),抗HIV硫代磷酸适体PS-d(T2G4T2)的不同G-四链体的影响并通过紫外热熔(Tm)和圆二色性(CD)实验研究了DNA端粒序列d(G4T4G4)。通常,用2'F-araG取代具有反构象的脱氧鸟嘌呤(抗鸟嘌呤)可以稳定G四元组并保持四链体构象,而用2'F-araG代替顺鸟嘌呤则不受欢迎,并且会导致戏剧性地切换到替代的四链体构象。已发现将2'F-araG或T残基掺入凝血酶结合的DNA G-四链体可使复合物稳定(ΔTm直至〜+ 3°C / 2'F-araN修饰)。 2'F-araN单位还将10%胎牛血清(FBS)的半衰期延长了48倍。如通过硝酸纤维素滤膜结合试验评估的那样,两种修饰的凝血酶结合适体(PG13和PG14)显示出与凝血酶的结合亲和力提高了约4倍,二者均具有提高的热稳定性(〜1°C / 2'F-ANA修饰) Tm升高)和核酸酶抗性(4-7倍)。因此,2'-脱氧-2'-氟-d-阿拉伯核糖核酸(2'F-ANA)修饰非常适合于调节(并改善)天然DNA G四联体的理化和生物学特性。

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