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胸腺嘧啶乙二醇损伤在体外可终止DNA聚合酶I的链延伸。

Thymine glycol lesions terminate chain elongation by DNA polymerase I in vitro.

作者信息

Clark J M, Beardsley G P

出版信息

Nucleic Acids Res. 1986 Jan 24;14(2):737-49. doi: 10.1093/nar/14.2.737.

Abstract

Single-strand circular DNA from bacteriophage M13mp9 was chemically modified with osmium tetroxide to introduce specifically cis-thymine glycol lesions, a major type of DNA damage produced by ionizing radiation. An oligonucleotide primer was extended on damaged and undamaged templates using either the large fragment of E. coli pol I or T4 DNA polymerase. The reaction products were analysed by electrophoresis alongside a DNA sequence ladder. Synthesis on the damaged templates terminated at positions opposite thymine bases in the template. These results indicate that cis-thymine glycol lesions in single-strand DNA constitute blocks to synthesis by DNA polymerases in vitro. Surprisingly, replication halts after the correct nucleotide, dAMP, is inserted opposite the lesion. These results imply that the primary effect of the thymine glycol lesion is suppression of DNA synthesis and that the lesion is not a potent mutagen.

摘要

用四氧化锇对来自噬菌体M13mp9的单链环状DNA进行化学修饰,以特异性引入顺式胸腺嘧啶二醇损伤,这是电离辐射产生的主要DNA损伤类型。使用大肠杆菌DNA聚合酶I的大片段或T4 DNA聚合酶,在受损和未受损模板上延伸寡核苷酸引物。反应产物与DNA序列梯一起通过电泳进行分析。在受损模板上的合成在模板中胸腺嘧啶碱基相对的位置终止。这些结果表明,单链DNA中的顺式胸腺嘧啶二醇损伤在体外构成了DNA聚合酶合成的障碍。令人惊讶的是,在损伤相对位置插入正确的核苷酸dAMP后,复制停止。这些结果表明胸腺嘧啶二醇损伤的主要作用是抑制DNA合成,并且该损伤不是一种强效诱变剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a656/339461/62f768c1e279/nar00271-0127-a.jpg

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