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一氧化氮在与电离辐射实现联合效应的过程中协调基因组不稳定性的发展。

Nitric oxide coordinates development of genomic instability in realization of combined effect with ionizing radiation.

作者信息

Mikhailenko V M, Diomina E A, Muzalov I I, Gerashchenko B I

机构信息

R.E. Kavetsky Institute of Experimental Pathology, Oncology and Radiobiology, NAS of Ukraine, Kyiv 03022, Ukraine.

出版信息

Exp Oncol. 2013 Mar;35(1):58-64.

Abstract

UNLABELLED

The aim of this study was to investigate the ability of environmental nitrogen oxides or natural nitric oxide (NO) donors to modify free radicals ba-lance and development of genomic instability alone or in combination with ionizing radiation.

METHODS

Genotoxicity and cytogenetic abnormalities were assessed in vitro in peripheral blood lymphocytes (PBL) isolated from healthy humans or in vivo in rats PBL. Human PBL were treated with physiologically relevant NO donor - S-Nitrosoglutathione and X-ray irradiation. The inhalation treatment of animals with NO was carried out in chamber with purified gaseous NO mixed inside with air. Levels of S-Nitrosohemoglobin and methemoglobin in the blood were assessed with electron paramagnetic resonance. The total level of reactive oxygen and nitrogen species in PBL was determined fluorometrically, and serum levels of reactive oxygen species was determined by spectrophotometric assay. DNA damages were assessed by alkaline single-cell gel electrophoresis. The frequency of chromosomal aberrations in human PBL measured with the conventional cytogenetic assay in metaphase cells on short-term (52 h) and long-term (72 h) cultures.

RESULTS

Environmental nitrogen oxides or release of NO from stable complexes with biomolecules (such as S-Nitrosothiols) intensified generation of free radicals, DNA damage and development of genomic instability alone or in combination with ionizing radiation. Treatment of PBL by S-Nitrosoglutathione caused prevalent induction of chromatid type but irradiation - chromosome aberrations. The dose dependence of chromatid-type aberrations observed in human PBL after combined influence of S-Nitrosoglutathione and ionizing radiation indicates a crucial role of NO in the formation of chromosomal instability.

CONCLUSION

NO can deregulate free radicals balance resulted in genotoxic effect, posttranslational modification of repair enzymes and thus coordinated development of genomic instability and increase of cancer risk.

摘要

未标记

本研究的目的是调查环境氮氧化物或天然一氧化氮(NO)供体单独或与电离辐射联合改变自由基平衡和基因组不稳定性发展的能力。

方法

在体外对从健康人分离的外周血淋巴细胞(PBL)或体内对大鼠PBL评估遗传毒性和细胞遗传学异常。用人PBL进行生理相关的NO供体——S-亚硝基谷胱甘肽和X射线照射处理。在装有与空气混合的纯化气态NO的舱室中对动物进行NO吸入处理。用电子顺磁共振评估血液中S-亚硝基血红蛋白和高铁血红蛋白的水平。用荧光法测定PBL中活性氧和氮物种的总水平,用分光光度法测定血清中活性氧物种的水平。通过碱性单细胞凝胶电泳评估DNA损伤。用传统细胞遗传学方法在中期细胞的短期(52小时)和长期(72小时)培养中测量人PBL中的染色体畸变频率。

结果

环境氮氧化物或NO从与生物分子的稳定复合物(如S-亚硝基硫醇)中的释放单独或与电离辐射联合增强了自由基的产生、DNA损伤和基因组不稳定性的发展。用S-亚硝基谷胱甘肽处理PBL导致染色单体型畸变普遍诱导,但照射导致染色体畸变。在S-亚硝基谷胱甘肽和电离辐射联合影响后人PBL中观察到的染色单体型畸变的剂量依赖性表明NO在染色体不稳定性形成中起关键作用。

结论

NO可失调自由基平衡,导致遗传毒性效应、修复酶的翻译后修饰,从而协调基因组不稳定性的发展和癌症风险的增加。

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