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父本F0生殖系照射后,ATM杂合性对小鼠可遗传DNA损伤的影响。

Effect of ATM heterozygosity on heritable DNA damage in mice following paternal F0 germline irradiation.

作者信息

Baulch Janet E, Li Ming-Wen, Raabe Otto G

机构信息

University of Maryland, Baltimore, Radiation Oncology Research Laboratory, BRB 7-002, 655 West Baltimore Street, Baltimore, MD 21201, USA.

出版信息

Mutat Res. 2007 Mar 1;616(1-2):34-45. doi: 10.1016/j.mrfmmm.2006.11.020. Epub 2006 Dec 11.

Abstract

The ataxia telangiectasia mutated (ATM) gene product maintains genome integrity and initiates cellular DNA repair pathways following exposures to genotoxic agents. ATM also plays a significant role in meiotic recombination during spermatogenesis. Fertilization with sperm carrying damaged DNA could lead to adverse effects in offspring including developmental defects or increased cancer susceptibility. Currently, there is little information regarding the effect of ATM heterozygosity on germline DNA repair and heritable effects of paternal germline-ionizing irradiation. We used neutral pH comet assays to evaluate spermatozoa 45 days after acute whole-body irradiation of male mice (0.1Gy, attenuated (137)Cs gamma rays) to determine the effect of ATM heterozygosity on delayed DNA damage effects of Type A/B spermatogonial irradiation. Using the neutral pH sperm comet assay, significant irradiation-related differences were found in comet tail length, percent tail DNA and tail extent moment, but there were no observed differences in effect between wild-type and ATM +/- mice. However, evaluation of spermatozoa from third generation descendants of irradiated male mice for heritable chromatin effects revealed significant differences in DNA electrophoretic mobility in the F(3) descendants that were based upon the irradiated F(0) sire's genotype. In this study, radiation-induced chromatin alterations to Type A/B spermatogonia, detected in mature sperm 45 days post-irradiation, led to chromatin effects in mature sperm three generations later. The early cellular response to and repair of DNA damage is critical and appears to be affected by ATM zygosity. Our results indicate that there is potential for heritable genetic or epigenetic changes following Type A/B spermatogonial irradiation and that ATM heterozygosity increases this effect.

摘要

共济失调毛细血管扩张症突变(ATM)基因产物可维持基因组完整性,并在暴露于基因毒性剂后启动细胞DNA修复途径。ATM在精子发生过程中的减数分裂重组中也起着重要作用。用携带受损DNA的精子受精可能会对后代产生不良影响,包括发育缺陷或癌症易感性增加。目前,关于ATM杂合性对生殖系DNA修复的影响以及父系生殖系电离辐射的遗传效应的信息很少。我们使用中性pH彗星试验来评估雄性小鼠急性全身照射(0.1Gy,衰减的(137)Csγ射线)45天后的精子,以确定ATM杂合性对A型/ B型精原细胞照射延迟DNA损伤效应的影响。使用中性pH精子彗星试验,在彗星尾长、尾DNA百分比和尾延伸矩方面发现了与辐射相关的显著差异,但在野生型和ATM +/-小鼠之间未观察到效应差异。然而,对受辐照雄性小鼠第三代后代的精子进行遗传染色质效应评估发现,F(3)后代的DNA电泳迁移率存在显著差异,这取决于受辐照的F(0)父本的基因型。在这项研究中,辐射诱导的A型/ B型精原细胞染色质改变在辐照后45天在成熟精子中被检测到,导致三代后成熟精子中的染色质效应。DNA损伤的早期细胞反应和修复至关重要,并且似乎受ATM纯合性的影响。我们的结果表明,A型/ B型精原细胞照射后存在遗传或表观遗传变化的可能性,并且ATM杂合性会增加这种效应。

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