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Base Analogs as Intrinsic Labels for the Study of DNA Structure by Fluorescence Resonance Energy Transfer

机译:基础类似物作为荧光共振能量转移研究DNA结构的内在标签

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Distance measurements using fluorescence resonance energy transfer (FRET) have been extensively applied to structural studies of proteins and protein:protein complexes. Only in a few instances FRET has been used for distance determination in oligonucleotides or oligonucleotide:protein complexes. In most of these studies donor acceptor systems with labels attached to the 5' ends of the individual oligonucleotide strands have been used. Since long flexible linkers are used to attach the dyes to the phosphate backbone of the oligonucleotide it is advantageous to analyze the experimental data in terms of a distribution of donor acceptor distances instead of a single distance. However, the length and the high flexibility of the linker arms result in broad distributions unsatisfactory for high precision distance determinations. In this study intrinsic labels like 2-aminopurine or dimethyllumazine are utilized instead. These fluorescent base analogs are incorporated into the DNA oligonucleotides and their viability for FRET measurements is tested. Time-domain measurements on oligonucleotides with one intrinsic label and one extrinsic label show that the recovered distance distributions are narrower. This improvement may even be enhanced by using intrinsic probes both as donor and as acceptor.
机译:使用荧光共振能量转移(FRET)的距离测量已广泛应用于蛋白质和蛋白质的结构研究:蛋白质复合物。仅在几个情况下,FRET已被用于寡核苷酸或寡核苷酸中的距离测定:蛋白质复合物。在大多数这些研究中,已经使用了附着于各个寡核苷酸链的5'末端的标签的供体受体系统。由于长期柔性接头用于将染料连接到寡核苷酸的磷酸盐骨架上,因此有利于分析供体受体距离的分布而不是单距离的实验数据。然而,接头臂的长度和高柔韧性导致广泛的分布对于高精度距离测定不令人满意。在该研究中,使用如2-氨基嘌呤或二甲基林碱等内在标记。将这些荧光基础类似物掺入DNA寡核苷酸中,并测试其用于摩擦测量的可行性。具有一个内在标记的寡核苷酸的时域测量和一个内在标记表明回收的距离分布较窄。通过使用作为供体和受体的固有探针甚至可以增强这种改进。

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