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Mutagenesis mediated by triple helix-forming oligonucleotides conjugated to psoralen: Effects of linker arm length and sequence context

机译:补骨脂素偶联的三螺旋形成寡核苷酸介导的诱变:接头臂长度和序列背景的影响。

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摘要

Targeted mutagenesis and gene knock-out can he mediated by triple helix-forming oligonucleotides (TFO) linked to mutagenic agents, such as psoralen, However, this strategy is limited by the availability of homopurine/homopyrimidine stretches at or near the target site because such sequences are required for high-affinity triplex formation, To overcome this limitation, we have tested TFO conjugated to psoralen via linker arms of lengths varying from 2 to 86 bonds, thereby designed to deliver the psoralen at varying distances from the third strand binding site present at the 3' end of the supFG1 mutation reporter gene. Following tripler formation and UVA irradiation, mutations were detected using an SV40-based shuttle vector assay in human cells, The frequency and distribution of mutations depended on the length of the linker arm, Precise targeting was observed only for linker arms of length 2 and 6, which also yielded the highest mutation frequencies (3 and 14%, respectively), Psoralen-TFO with longer tethers yielded mutations at multiple sites, with the maximum distance from the tripler site limited by the linker length but with the distribution within that range influenced by the propensity for psoralen intercalation at A:T base-pair-rich sites, Thus, gene modification can be extended beyond the site of third strand binding but with a decrease in the precision of the targeting. [References: 19]
机译:靶向诱变和基因敲除可以由与诱变剂(例如补骨脂素)相连的三螺旋形成寡核苷酸(TFO)介导。但是,这种策略受到靶位点或附近的高嘌呤/高嘧啶片段的可用性的限制,因为序列是高亲和力三链体形成所必需的,为了克服这一限制,我们已经测试了通过2至86个键长不等的连接臂与补骨脂素缀合的TFO,从而设计为在距存在的第三链结合位点不同距离处输送补骨脂素在supFG1突变报告基因的3'末端。在三聚体形成和UVA照射后,使用基于SV40的穿梭载体测定法在人细胞中检测到突变,突变的频率和分布取决于接头臂的长度,仅对长度为2和6的接头臂观察到精确的靶向,它也产生最高的突变频率(分别为3%和14%),带有较长束缚的Psoralen-TFO在多个位点产生突变,与三聚体位点的最大距离受到接头长度的限制,但该范围内的分布会受到影响由于补骨脂素在富含A:T碱基对的位点上的插入倾向,因此,基因修饰可扩展到第三链结合位点之外,但降低了靶向的精度。 [参考:19]

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