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A modified single-strand annealing model best explains the joining of DNA double-strand breaks mammalian cells and cell extracts.

机译:改进的单链退火模型可以最好地解释DNA双链断裂与哺乳动物细胞和细胞提取物的结合。

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摘要

The joining of DNA double-strand breaks in vivo is frequently accompanied by the loss of a few nucleotides at the junction between the interacting partners. In vitro systems mimic this loss and, on detailed analysis, have suggested two models for the mechanism of end-joining. One invokes the use of extensive homologous side-by-side alignment of the partners prior to joining, while the other proposes the use of small regions of homology located at or near the terminus of the interacting molecules. to discriminate between these two models, assays were conducted both in vitro and in vivo with specially designed substrates. In vitro, molecules with limited terminal homology were capable of joining, but analysis of the junctions suggested that the mechanism employed the limited homology available. In vivo, the substrates with no extensive homology end-joined with equal efficiency to those with extensive homology in two different topological arrangements. Taken together, these results suggest that extensive homology is not a prerequisite for efficient end-joining, but that small homologies close to the terminus are used preferentially, as predicted by the modified single-strand annealing model.
机译:体内DNA双链断裂的连接经常伴随着相互作用伴侣之间连接处的几个核苷酸的丢失。体外系统模拟了这种损失,并且在详细分析中提出了两种末端连接机理的模型。一种方法是在连接之前调用伴侣的广泛同源并排比对,另一种则建议使用位于相互作用分子末端或附近的小同源性区域。为了区分这两种模型,使用专门设计的底物在体外和体内进行了测定。在体外,具有有限末端同源性的分子能够连接,但是对连接的分析表明该机制采用了可用的有限同源性。在体内,没有广泛同源性的底物在两个不同的拓扑结构中以与具有广泛同源性的底物相同的效率末端连接。综上所述,这些结果表明,广泛的同源性不是高效末端连接的先决条件,但是,如改良的单链退火模型所预测的,优选优先使用靠近末端的小同源性。

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