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DNA sequence preferences of several AT-selective minor groove binding ligands.

机译:几种AT选择性小沟结合配体的DNA序列偏好。

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摘要

We have examined the interaction of distamycin, netropsin, Hoechst 33258 and berenil, which are AT-selective minor groove-binding ligands, with synthetic DNA fragments containing different arrangements of AT base pairs by DNase I footprinting. For fragments which contain multiple blocks of (A/T)4 quantitative DNase I footprinting reveals that AATT and AAAA are much better binding sites than TTAA and TATA. Hoechst 33258 shows that greatest discrimination between these sites with a 50-fold difference in affinity between AATT and TATA. Alone amongst these ligands, Hoechst 33258 binds to AATT better than AAAA. These differences in binding to the various AT-tracts are interpreted in terms of variations in DNA minor groove width and suggest that TpA steps within an AT-tract decrease the affinity of these ligands. The behaviour of each site also depends on the flanking sequences; adjacent pyrimidine-purine steps cause a decrease in affinity. The precise ranking order for the various binding sites is not the same for each ligand.
机译:我们已经检查了脱氨霉素,netropsin,Hoechst 33258和berenil(它们是AT选择性小沟结合配体)与通过DNase I足迹合成的包含不同AT碱基对排列的合成DNA片段的相互作用。对于包含多个(A / T)4定量DNase片段的片段,足迹表明AATT和AAAA是比TTAA和TATA更好的结合位点。 Hoechst 33258表明,这些位点之间的最大区别是AATT与TATA之间的亲和力相差50倍。在这些配体中,Hoechst 33258与AATT的结合优于AAAA。这些与各种AT束结合的差异是根据DNA小沟宽度的变化来解释的,表明AT束中的TpA步骤会降低这些配体的亲和力。每个位点的行为也取决于侧翼序列。相邻的嘧啶-嘌呤步骤会导致亲和力降低。对于每个配体,各种结合位点的精确排序顺序都不相同。

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