Nikiforov V S, Blinova E A, Kotikova A I, Akleyev A V
Urals Research Center for Radiation Medicine, Chelyabinsk, Russia.
Vavilovskii Zhurnal Genet Selektsii. 2022 Feb;26(1):50-58. doi: 10.18699/VJGB-22-08.
Transcriptional activity of genes involved in maintaining genetic homeostasis (genes for repair, cell cycle and apoptosis: TP53, MDM2, ATM, BAX, BCL-2, CDKN1A, OGG1, XPC, PADI4, MAPK8, NF-KB1, STAT3, GATA3) was studied in chronically exposed persons with an increased intensity of early and late stages of apoptosis and necrosis of peripheral blood lymphocytes. The object of this study was peripheral blood mononuclear cells obtained from 132 chronically exposed residents of the Techa riverside villages. The mean accumulated dose to red bone marrow was 426.4 ± 48.2 mGy (1.3-2930.0 mGy), to thymus and peripheral immune organs, 58.9 ± 7.9 mGy (0.1-489.0 mGy). The study was performed more than 60 years after the onset of exposure, the average age of exposed persons was 68 ± 0.6 years (55-86 years). The study of apoptotic and necrotic death of peripheral blood lymphocytes was based on the presence of phosphatidylserine on the cell membrane surface, as well as on its permeability for DNA-intercalating dye. Evaluation of the relative content of mRNA genes for repair, cell cycle, and apoptosis was carried out using real-time PCR. An increased relative content of PADI4 gene mRNA was registered in the group of chronically exposed persons with the increased intensity of early apoptosis (p = 0.006). Modulation of the relative content of mRNA of the TP53 (p = 0.013) and BCL-2 (p = 0.021) genes was detected in the group of chronically exposed individuals with the increased intensity of the late stage of apoptosis. A statistically signif icant increase in the transcriptional activity of the TP53 gene was observed in the group of chronically exposed persons with the increased intensity of peripheral blood lymphocyte necrosis in the long-term period (p = 0.015). In the course of the study it was noted that exposed people with increased intensity of apoptosis, f irst of all, demonstrate changes in the transcriptional activity of apoptotic genes. These data are consistent with current views on the activation of programmed cell death.
在慢性暴露个体中,研究了参与维持基因稳态的基因(修复、细胞周期和凋亡相关基因:TP53、MDM2、ATM、BAX、BCL-2、CDKN1A、OGG1、XPC、PADI4、MAPK8、NF-KB1、STAT3、GATA3)的转录活性,这些个体外周血淋巴细胞早期和晚期凋亡及坏死强度增加。本研究的对象是从捷恰河畔村庄的132名长期暴露居民中获取的外周血单个核细胞。红骨髓的平均累积剂量为426.4±48.2 mGy(1.3 - 2930.0 mGy),胸腺和外周免疫器官的平均累积剂量为58.9±7.9 mGy(0.1 - 489.0 mGy)。该研究在暴露开始60多年后进行,暴露个体的平均年龄为68±0.6岁(55 - 86岁)。外周血淋巴细胞凋亡和坏死死亡的研究基于细胞膜表面磷脂酰丝氨酸的存在以及其对DNA嵌入染料的通透性。使用实时PCR评估修复、细胞周期和凋亡相关基因mRNA的相对含量。在早期凋亡强度增加的慢性暴露个体组中,检测到PADI4基因mRNA的相对含量增加(p = 0.006)。在晚期凋亡强度增加的慢性暴露个体组中,检测到TP53(p = 0.013)和BCL-2(p = 0.021)基因mRNA相对含量的调节。在长期外周血淋巴细胞坏死强度增加的慢性暴露个体组中,观察到TP53基因的转录活性有统计学意义的增加(p = 0.015)。在研究过程中注意到,凋亡强度增加的暴露个体首先表现出凋亡基因转录活性的变化。这些数据与当前关于程序性细胞死亡激活的观点一致。
