PEITC Induces DNA Damage and Inhibits DNA Repair-Associated Proteins in Human Retinoblastoma Cells In Vitro

IF 4.4 3区 医学 Q2 ENVIRONMENTAL SCIENCES Environmental Toxicology Pub Date : 2024-08-23 DOI:10.1002/tox.24393
Sheng-Yao Hsu, Yi-Ping Huang, Te-Chun Hsia, Jaw-Chyun Chen, Shu-Fen Peng, Wen-Tsong Hsieh, Fu-Shin Chueh, Chao-Lin Kuo
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Abstract

Phenethyl isothiocyanate (PEITC), a natural product, exists in biological activities, including anticancer activity in many human cancer cells. No information shows that PEITC affects DNA damage in human retinoblastoma (RB) cells in vitro. In this study, the aim of experiments was to determine whether PEITC decreased total viable cell number or not by inducing protein expressions involved in DNA damage and repair in Y79 RB cells in vitro. Total cell viability was measured by PI exclusion assay, and PEITC reduced the total Y79 viable cell numbers in a dose-dependent manner. DNA condensation and DNA impairment were conducted by DAPI staining and comet assays, respectively, in Y79 cells. The findings show that PEITC induced DNA condensation dose-dependently based on the brighter fluorescence of cell nuclei stained by DAPI staining. PEITC-induced DNA damage showed a more extended DNA migration smears than that of the control, which was performed by a comet assay. Western blotting was performed to measure the protein expressions involved in DNA damage and repair, which showed that PEITC at 2.5–10 μM increased NRF2, HO-1, SOD (Mn), and catalase; however, it decreased SOD (Cu/Zn) except 10 μM PEITC treatment, and decreased glutathione, which were associated with oxidative stress. Furthermore, PEITC increased DNA-PK, MDC1, H2A.XpSer139, ATMpSer1981, p53, p53pSer15, PARP, HSP70, and HSP90, but decreased TOPIIα, TOPIIβ, and MDM2pSer166 that were associated with DNA damage and repair mechanism in Y79 cells. The examination from confocal laser microscopy shows that PEITC increased H2A.XpSer139 and p53pSer15, and decreased glutathione and TOPIIα in Y79 cells. In conclusion, the cytotoxic effects of PEITC on reducing the number of viable cells may be due to the induction of DNA damage and the alteration of DNA repair proteins in Y79 cells in vitro.

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PEITC 诱导 DNA 损伤并抑制体外人类视网膜母细胞瘤细胞中的 DNA 修复相关蛋白
异硫氰酸苯乙酯(PEITC)是一种天然产品,具有多种生物活性,包括对许多人类癌细胞的抗癌活性。目前还没有资料显示 PEITC 在体外影响人类视网膜母细胞瘤(RB)细胞的 DNA 损伤。本研究的目的是确定 PEITC 是否会通过诱导 Y79 RB 细胞中参与 DNA 损伤和修复的蛋白质表达来减少细胞的总存活数。实验采用 PI 排除法测定细胞的总存活率,PEITC 以剂量依赖的方式减少了 Y79 存活细胞的总数。通过 DAPI 染色和彗星试验分别检测了 Y79 细胞的 DNA 缩合和 DNA 损伤。研究结果表明,根据 DAPI 染色后细胞核荧光的亮度,PEITC 诱导的 DNA 缩合与剂量有关。彗星试验显示,与对照组相比,PEITC 诱导的 DNA 损伤显示出更长的 DNA 迁移涂片。Western印迹法测定了参与DNA损伤和修复的蛋白质表达,结果表明,2.5-10 μM的PEITC可增加NRF2、HO-1、SOD(锰)和过氧化氢酶;但除10 μM PEITC处理外,SOD(铜/锌)降低,谷胱甘肽降低,这与氧化应激有关。此外,PEITC 增加了 Y79 细胞中与 DNA 损伤和修复机制相关的 DNA-PK、MDC1、H2A.XpSer139、ATMpSer1981、p53、p53pSer15、PARP、HSP70 和 HSP90,但减少了 TOPIIα、TOPIIβ 和 MDM2pSer166。激光共聚焦显微镜检查显示,PEITC 增加了 Y79 细胞中的 H2A.XpSer139 和 p53pSer15,降低了谷胱甘肽和 TOPIIα。总之,PEITC 对减少存活细胞数量的细胞毒性作用可能是由于在体外诱导了 Y79 细胞的 DNA 损伤和 DNA 修复蛋白的改变。
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来源期刊
Environmental Toxicology
Environmental Toxicology 环境科学-毒理学
CiteScore
7.10
自引率
8.90%
发文量
261
审稿时长
4.5 months
期刊介绍: The journal publishes in the areas of toxicity and toxicology of environmental pollutants in air, dust, sediment, soil and water, and natural toxins in the environment.Of particular interest are: Toxic or biologically disruptive impacts of anthropogenic chemicals such as pharmaceuticals, industrial organics, agricultural chemicals, and by-products such as chlorinated compounds from water disinfection and waste incineration; Natural toxins and their impacts; Biotransformation and metabolism of toxigenic compounds, food chains for toxin accumulation or biodegradation; Assays of toxicity, endocrine disruption, mutagenicity, carcinogenicity, ecosystem impact and health hazard; Environmental and public health risk assessment, environmental guidelines, environmental policy for toxicants.
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