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咪唑环开环的DNA嘌呤及其生物学意义。

Imidazole ring-opened DNA purines and their biological significance.

作者信息

Tudek Barbara

机构信息

Institute of Biochemistry and Biophysics, Polish Academy of Sciences, 02-106 Warsaw, Poland.

出版信息

J Biochem Mol Biol. 2003 Jan 31;36(1):12-9. doi: 10.5483/bmbrep.2003.36.1.012.

Abstract

Fragmentation of purine imidazole ring and production of formamidopyrimidines in deoxynucleosides (Fapy lesions) occurs upon DNA oxidation as well as upon spontaneous or alkali-triggered rearrangement of certain alkylated bases. Many chemotherapeutic agents such as cyclophosphamide or thiotepa produce such lesions in DNA. Unsubstituted FapyA and FapyG, formed upon DNA oxidation cause moderate inhibition of DNA synthesis, which is DNA polymerase and sequence dependent. Fapy-7MeG, a methylated counterpart of FapyG-, a efficiently inhibits DNA replication in vitro and in E.coli, however its mutagenic potency is low. This is probably due to preferential incorporation of cytosine opposite Fapy-7MeG and preferential extension of Fapy-7MeG:C pair. In contrast, FapyA and Fapy-7MeA possess miscoding potential. Both lesions in SOS induced E.coli preferentially mispair with cytosine giving rise to A-->G transitions. Fapy lesions substituted with longer chain alkyl groups also show simult aneous lethal and mutagenic properties. Fapy lesions are actively eliminated from DNA by repair glycosylases specific for oxidized purines and pyrimidines both in bacteria and eukaryotic cells. Bacterial enzymes include E.coli formamidopyrimidine-DNA-glycosylase (Fpg protein), endonuclease III (Nth protein) and endonuclease VIII (Nei protein).

摘要

嘌呤咪唑环的断裂以及脱氧核苷中氨甲酰嘧啶的产生(Fapy损伤)在DNA氧化时发生,也在某些烷基化碱基的自发或碱引发的重排过程中出现。许多化疗药物,如环磷酰胺或噻替哌,会在DNA中产生此类损伤。DNA氧化时形成的未取代的FapyA和FapyG会对DNA合成产生中度抑制,这种抑制取决于DNA聚合酶和序列。FapyG的甲基化对应物Fapy - 7MeG在体外和大肠杆菌中能有效抑制DNA复制,但其诱变能力较低。这可能是由于在Fapy - 7MeG对面优先掺入胞嘧啶以及Fapy - 7MeG:C碱基对的优先延伸。相比之下,FapyA和Fapy - 7MeA具有错配编码潜力。在SOS诱导的大肠杆菌中,这两种损伤都优先与胞嘧啶错配,导致A→G转换。被较长链烷基取代的Fapy损伤也同时具有致死和诱变特性。在细菌和真核细胞中,Fapy损伤可被针对氧化嘌呤和嘧啶的修复糖基化酶从DNA中有效清除。细菌酶包括大肠杆菌氨甲酰嘧啶 - DNA - 糖基化酶(Fpg蛋白)、核酸内切酶III(Nth蛋白)和核酸内切酶VIII(Nei蛋白)。

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