首页> 外文期刊>Nucleic Acids Research >TRANS-COMPLEMENTATION BY HUMAN APURINIC ENDONUCLEASE (APE) OF HYPERSENSITIVITY TO DNA DAMAGE AND SPONTANEOUS MUTATOR PHENOTYPE IN APN1(-)YEAST
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TRANS-COMPLEMENTATION BY HUMAN APURINIC ENDONUCLEASE (APE) OF HYPERSENSITIVITY TO DNA DAMAGE AND SPONTANEOUS MUTATOR PHENOTYPE IN APN1(-)YEAST

机译:人类对APN1(-)酵母对DNA损伤和自发突变型表型的超敏性的人类固有核糖核酸酶(APE)的反转录补体

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摘要

Abasic (AP) sites in DNA are potentially lethal and mutagenic. Class II' AP endonucleases initiate the repair of these and other DNA lesions, In yeast, the predominant enzyme of this type is Apn1, and its elimination sensitizes the cells to killing by simple alkylating agents or oxidants, and raises the rate of spontaneous mutation, We investigated the ability of the major human class II AP endonuclease, Ape, which is structurally unrelated to Apn1, to replace the yeast enzyme in vivo, Confocal immunomicroscopy studies indicate that similar to 25% of the Ape expressed in yeast is present in the nucleus, High-level Ape expression corresponding to similar to 7000 molecules per nucleus, equal to the normal Apn1 copy number, restored resistance to methyl methanesulfonate to near wild-type levels in Apn1-deficient (apn1(-)) yeast, Ape expression in apn1(-) yeast provided little protection against H2O2 challenges, consistent with the weak 3'-repair diesterase activity of the human enzyme, Ape expression at similar to 2000 molecules per nucleus reduced the spontaneous mutation rate of apn1(-) yeast to that seen for wild-type cells, Because Ape has a powerful AP endonuclease but weak 3'-diesterase activity, these findings indicate that endogenously generated AP sites can drive spontaneous mutagenesis.
机译:DNA中的无碱基(AP)位点可能具有致死性和致突变性。 II类AP内切核酸酶开始修复这些和其他DNA损伤。在酵母中,这种类型的主要酶是Apn1,其消除使细胞对简单的烷基化剂或氧化剂的杀伤敏感,并提高了自发突变的频率,我们研究了结构上与Apn1不相关的主要人类II类AP核酸内切酶Ape替代体内酵母酶的能力,共聚焦免疫显微镜研究表明,核中存在与酵母中表达的Ape相似的25% ,相当于每个核中有7000个分子的高水平Ape表达,等于正常的Apn1拷贝数,在Apn1缺陷型(apn1(-))酵母中将对甲磺酸甲酯的抗性恢复到接近野生型水平,而apn1中的Ape表达(-)酵母几乎没有针对H2O2攻击的保护作用,这与人类酶的弱3'-修复二酯酶活性相一致,每个核的Ape表达类似于2000个分子,降低了t他将apn1(-)酵母的自发突变率设为野生型细胞,因为Ape具有强大的AP核酸内切酶但弱的3'-二酯酶活性,这些发现表明内源性产生的AP位点可以驱动自发诱变。

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