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突变特异性与切除修复的影响:对错误避免和错误修复机制的见解

Mutational specificity and the influence of excision repair: insights into the mechanisms of error-avoidance and error-fixation.

作者信息

Glickman B W

机构信息

Department of Biology, York University, Toronto, Ont., Canada.

出版信息

Genome. 1989;31(2):584-9. doi: 10.1139/g89-108.

DOI:10.1139/g89-108
PMID:2698833
Abstract

The excision repair process controlled by the uvrABC gene in Escherichia coli is the major pathway for the repair of a diverse series of DNA damages. To achieve a better understanding of the mechanics of this repair pathway and its impact upon mutagenesis, we have applied a recently developed technology by which the nature of mutation is determined at the DNA sequence level. A comparison of the classes and distribution of mutation in excision-repair-proficient and excision-repair-deficient strains of E. coli reveals that the absence of excision repair can alter both the nature of the mutations recovered as well as their distribution. This can occur in one of several ways. For example, under some circumstances the action of the UvrABC pathway can lead to interruptions of DNA strand continuity and an enhancement of both frameshift and deletion events. Such an effect is seen following damage by psoralen plus near UV (PUVA) treatment that produces crosslinks in the DNA. In comparison, several other treatments produce similar distributions within the classes of mutations recovered but demonstrate an alteration in site specificity. Such is the case following UV irradiation. In this case, the data indicate that while the premutagenic lesions may be the same, mutation fixation in the presence and absence of excision repair may involve different mechanisms. Similarly, evidence from the repair of damage by ethylating agents indicates that while the nature of the mutations recovered is not altered, the preferred location of these events is altered in the absence of excision repair. These results indicate that local DNA sequence can affect on the efficiency of excision repair.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

大肠杆菌中由uvrABC基因控制的切除修复过程是修复多种DNA损伤的主要途径。为了更好地理解这一修复途径的机制及其对诱变的影响,我们应用了一项最近开发的技术,通过该技术可以在DNA序列水平上确定突变的性质。对大肠杆菌切除修复 proficient和切除修复缺陷菌株中突变的类别和分布进行比较后发现,切除修复的缺失既能改变所恢复突变的性质,也能改变其分布。这可以通过几种方式之一发生。例如,在某些情况下,UvrABC途径的作用会导致DNA链连续性的中断,并增加移码和缺失事件。在用补骨脂素加近紫外线(PUVA)处理造成DNA交联后会出现这种效果。相比之下,其他几种处理在所恢复的突变类别中产生相似的分布,但显示出位点特异性的改变。紫外线照射后就是这种情况。在这种情况下,数据表明,虽然诱变前的损伤可能相同,但在有和没有切除修复的情况下,突变固定可能涉及不同的机制。同样,来自烷化剂损伤修复的证据表明,虽然所恢复突变的性质没有改变,但在没有切除修复的情况下,这些事件的首选位置会发生改变。这些结果表明,局部DNA序列会影响切除修复的效率。(摘要截短为250字)

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