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Linkage structures strongly influence the binding cooperativity of DNA intercalators conjugated to triplex forming oligonucleotides.

机译:链接结构强烈影响与三重形成寡核苷酸缀合的DNA嵌入剂的结合协同作用。

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摘要

Conjugation of DNA intercalators to triple helix forming oligodeoxynucleotides (ODN's) can enhance ODN binding properties and consequently their potential ability to modulate gene expression. To test the hypothesis that linkage structure could strongly influence the binding enhancement of intercalator conjugation with triplex forming ODN's, we have used a model system to investigate binding avidity of short oligomers conjugated to DNA intercalators through various linkages. Using a dA10.T10 target sequence imbedded in a 20 bp duplex, binding avidities of a T10 ODN joined to the DNA intercalator 6,9-diamino, 3-methoxy acridine (DAMA) by 8 different 5' linkages were measured using an electrophoretic mobility shift assay. Although unmodified T10 has a very limited capacity for stable binding under these conditions (apparent Kd > 250 microM at 4 degrees C), conjugation to DAMA using flexible linkers of certain lengths and chemical compositions greatly enhanced binding (Kd of 1 microM at 4 degrees C). Other linkers, however, modestly enhanced binding or had no effect on binding at all. Thus, the length, flexibility, and chemical composition of linker structures all substantially influence intercalator conjugated oligodeoxynucleotide binding avidity.
机译:DNA嵌入剂与三重螺旋形成寡脱氧核苷酸(ODN's)的缀合可增强ODN结合特性,从而增强其调节基因表达的潜在能力。为了测试连接结构可以强烈影响嵌入剂与三链体形成ODN的结合增强的假设,我们使用了一个模型系统来研究通过各种连接与DNA嵌入剂结合的短寡聚物的结合亲和力。使用嵌入20 bp双链体的dA10.T10靶序列,使用电泳迁移率测量通过8个不同的5'键与DNA嵌入剂6,9-二氨基,3-甲氧基a啶(DAMA)连接的T10 ODN的结合亲和力位移测定。尽管未修饰的T10在这些条件下稳定结合的能力非常有限(在4°C下,表观Kd> 250 microM),但使用一定长度的柔性接头和化学成分与DAMA结合后,结合力大大增强(在4°C下,Kd为1 microM) )。然而,其他接头适度地增强了结合或根本不影响结合。因此,接头结构的长度,柔性和化学组成均基本上影响嵌入剂缀合的寡脱氧核苷酸结合亲和力。

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