The DNA damage response to radiological imaging: from ROS and γH2AX foci induction to gene expression responses in vivo.

IF 1.5 4区 环境科学与生态学 Q3 BIOLOGY Radiation and Environmental Biophysics Pub Date : 2023-08-01 DOI:10.1007/s00411-023-01033-4
Milagrosa López-Riego, Magdalena Płódowska, Milena Lis-Zajęcka, Kamila Jeziorska, Sylwia Tetela, Aneta Węgierek-Ciuk, Daniel Sobota, Janusz Braziewicz, Lovisa Lundholm, Halina Lisowska, Andrzej Wojcik
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Abstract

Candidate ionising radiation exposure biomarkers must be validated in humans exposed in vivo. Blood from patients undergoing positron emission tomography-computed tomography scan (PET-CT) and skeletal scintigraphy (scintigraphy) was drawn before (0 h) and after (2 h) the procedure for correlation analyses of the response of selected biomarkers with radiation dose and other available patient information. FDXR, CDKN1A, BBC3, GADD45A, XPC, and MDM2 expression was determined by qRT-PCR, DNA damage (γH2AX) by flow cytometry, and reactive oxygen species (ROS) levels by flow cytometry using the 2', 7'-dichlorofluorescein diacetate test in peripheral blood mononuclear cells (PBMC). For ROS experiments, 0- and 2-h samples were additionally exposed to UVA to determine whether diagnostic irradiation conditioned the response to further oxidative insult. With some exceptions, radiological imaging induced weak γH2AX foci, ROS and gene expression fold changes, the latter with good coherence across genes within a patient. Diagnostic imaging did not influence oxidative stress in PBMC successively exposed to UVA. Correlation analyses with patient characteristics led to low correlation coefficient values. γH2AX fold change, which correlated positively with gene expression, presented a weak positive correlation with injected activity, indicating a radiation-induced subtle increase in DNA damage and subsequent activation of the DNA damage response pathway. The exposure discrimination potential of these biomarkers in the absence of control samples as frequently demanded in radiological emergencies, was assessed using raw data. These results suggest that the variability of the response in heterogeneous populations might complicate identifying individuals exposed to low radiation doses.

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DNA损伤对放射成像的反应:从ROS和γH2AX病灶诱导到体内基因表达反应。
候选电离辐射暴露生物标志物必须在体内暴露的人体中进行验证。对接受正电子发射断层扫描-计算机断层扫描(PET-CT)和骨骼闪烁成像(scintigraphy)的患者在手术前(0小时)和手术后(2小时)抽取血液,分析所选生物标志物与辐射剂量和其他可用患者信息的相关性。采用qRT-PCR检测外周血单核细胞(PBMC)中FDXR、CDKN1A、BBC3、GADD45A、XPC和MDM2的表达,流式细胞术检测DNA损伤(γ - h2ax),流式细胞术检测2′,7′-二氯荧光素双醋酸酯试验检测活性氧(ROS)水平。在ROS实验中,将0和2小时的样品额外暴露于UVA,以确定诊断性照射是否会调节对进一步氧化损伤的反应。除了一些例外,放射成像诱导弱γH2AX灶,ROS和基因表达折叠变化,后者在患者内的基因间具有良好的一致性。诊断成像对连续暴露于UVA的PBMC的氧化应激无影响。与患者特征相关分析导致相关系数值较低。γ - h2ax折叠变化与基因表达呈正相关,与注射活性呈弱正相关,提示辐射诱导的DNA损伤轻微增加,随后激活DNA损伤反应途径。在没有对照样本的情况下,这些生物标志物的暴露识别潜力在放射紧急情况下经常被要求使用原始数据进行评估。这些结果表明,异质性人群中反应的可变性可能使识别暴露于低辐射剂量的个体复杂化。
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来源期刊
CiteScore
4.00
自引率
5.90%
发文量
53
审稿时长
>36 weeks
期刊介绍: This journal is devoted to fundamental and applied issues in radiation research and biophysics. The topics may include: Biophysics of ionizing radiation: radiation physics and chemistry, radiation dosimetry, radiobiology, radioecology, biophysical foundations of medical applications of radiation, and radiation protection. Biological effects of radiation: experimental or theoretical work on molecular or cellular effects; relevance of biological effects for risk assessment; biological effects of medical applications of radiation; relevance of radiation for biosphere and in space; modelling of ecosystems; modelling of transport processes of substances in biotic systems. Risk assessment: epidemiological studies of cancer and non-cancer effects; quantification of risk including exposures to radiation and confounding factors Contributions to these topics may include theoretical-mathematical and experimental material, as well as description of new techniques relevant for the study of these issues. They can range from complex radiobiological phenomena to issues in health physics and environmental protection.
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