The Interaction of Myeloperoxidase with the Industrial Contaminant 6-PPD: A Potential Pathway for Reactive Metabolites.

IF 3.7 3区 医学 Q2 CHEMISTRY, MEDICINAL Chemical Research in Toxicology Pub Date : 2024-10-21 Epub Date: 2024-10-03 DOI:10.1021/acs.chemrestox.4c00265
Steven Lockhart, Dinesh Babu, Newton H Tran, Béla Reiz, Lusine Tonoyan, Arno G Siraki
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Abstract

6-PPD (N-[1,3-dimethylbutyl]-N'-phenyl-p-phenylenediamine) is an industrial antioxidant reported to be an environmental contaminant. It was found to be highly toxic to coho salmon and potentially other aquatic organisms. The toxicity of 6-PPD in humans, however, remains unknown. The neutrophil enzyme myeloperoxidase (MPO) is known to catalyze xenobiotic metabolism; therefore, its role in 6-PPD cytotoxicity was investigated using the MPO-rich HL-60 cell line. UV-visible spectroscopy and liquid chromatography-mass spectrometry (LC/MS) were performed to investigate the MPO-mediated oxidation of 6-PPD and identify possible metabolites in the absence and presence of glutathione (GSH). 6-PPD's cytotoxicity, effect on mitochondrial membrane potential (MMP), and GSH-depleting ability in HL-60 cells were assessed. Electron paramagnetic resonance (EPR) was used to determine GSH radical formation using DMPO, and mitochondrial-derived superoxide was assessed with the mito-TEMPO-H probe. Evaluation of the 6-PPD-induced cellular injury pathways was performed by preincubating an antioxidant and an MPO inhibitor with HL-60 cells. UV-vis analysis of MPO-catalyzed oxidation of 6-PPD demonstrated changes in the 6-PPD spectrum, whereas the addition of GSH altered the spectrum, indicating possible GSH conjugate formation. LC/MS showed the formation of multiple products, including GSH-6-PPD conjugates and a GSH conjugate to a 4-hydroxydiphenylamine (a known 6-PPD degradant), which could potentially induce cytotoxicity. 6-PPD demonstrated concentration-dependent cytotoxicity, and cellular GSH levels were decreased by 6-PPD. Similarly, the level of MMP decreased, suggesting mitochondrial depolarization. Furthermore, the EPR spin probe for mitochondrial superoxide showed a positive relationship with 6-PPD concentration, and EPR spin-trapping demonstrated 6-PPD concentration-dependent GSH radical signal intensity using MPO/H2O2. The GSH precursor, NAC, demonstrated partial cytoprotection against 6-PPD; however, the MPO inhibitor PF-1355 surprisingly showed no significant cytoprotective effect. Our results suggest that MPO could be a potential catalyst for 6-PPD toxicity in humans. However, MPO inhibition did not significantly affect cellular viability, suggesting an MPO-independent toxicity pathway. These findings warrant a deeper investigation to determine 6-PPD mammalian toxicity pathways.

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髓过氧化物酶与工业污染物 6-PPD的相互作用:活性代谢物的潜在途径。
据报道,6-PPD(N-[1,3-二甲基丁基]-N'-苯基对苯二胺)是一种工业抗氧化剂,也是一种环境污染物。研究发现,它对鲑鱼和其他水生生物有剧毒。然而,6-PPD 对人体的毒性仍然未知。众所周知,中性粒细胞酶髓过氧化物酶(MPO)可催化异生物的新陈代谢;因此,我们使用富含 MPO 的 HL-60 细胞系研究了它在 6-PPD 细胞毒性中的作用。研究人员利用紫外-可见光谱法和液相色谱-质谱法(LC/MS)研究了 MPO 介导的 6-PPD 氧化作用,并确定了在谷胱甘肽(GSH)不存在和存在的情况下可能存在的代谢物。评估了 6-PPD 的细胞毒性、对线粒体膜电位(MMP)的影响以及在 HL-60 细胞中的 GSH 消耗能力。使用电子顺磁共振(EPR)测定了 DMPO 对 GSH 自由基形成的影响,并使用 mito-TEMPO-H 探针评估了线粒体衍生的超氧化物。通过将抗氧化剂和 MPO 抑制剂与 HL-60 细胞预孵育,对 6-PPD 诱导的细胞损伤途径进行了评估。对 MPO 催化的 6-PPD 氧化反应进行的紫外-可见光分析表明,6-PPD 的光谱发生了变化,而 GSH 的加入则改变了光谱,表明可能形成了 GSH 共轭物。LC/MS 显示形成了多种产物,包括 GSH-6-PPD 共轭物和 GSH 与 4-羟基二苯胺(已知的 6-PPD 降解剂)的共轭物,这可能会诱发细胞毒性。6-PPD 显示出浓度依赖性细胞毒性,细胞 GSH 水平因 6-PPD 而降低。同样,MMP 的水平也下降了,这表明线粒体去极化。此外,线粒体超氧化物的 EPR 自旋探针与 6-PPD 的浓度呈正相关,EPR 自旋捕获表明 6-PPD 的浓度与使用 MPO/H2O2 的 GSH 自由基信号强度有关。GSH 前体 NAC 对 6-PPD 具有部分细胞保护作用;但令人惊讶的是,MPO 抑制剂 PF-1355 未显示出明显的细胞保护作用。我们的研究结果表明,MPO 可能是 6-PPD 对人体毒性的潜在催化剂。然而,抑制 MPO 并未对细胞活力产生明显影响,这表明毒性途径与 MPO 无关。这些发现值得进行更深入的研究,以确定 6-PPD 在哺乳动物中的毒性途径。
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来源期刊
CiteScore
7.90
自引率
7.30%
发文量
215
审稿时长
3.5 months
期刊介绍: Chemical Research in Toxicology publishes Articles, Rapid Reports, Chemical Profiles, Reviews, Perspectives, Letters to the Editor, and ToxWatch on a wide range of topics in Toxicology that inform a chemical and molecular understanding and capacity to predict biological outcomes on the basis of structures and processes. The overarching goal of activities reported in the Journal are to provide knowledge and innovative approaches needed to promote intelligent solutions for human safety and ecosystem preservation. The journal emphasizes insight concerning mechanisms of toxicity over phenomenological observations. It upholds rigorous chemical, physical and mathematical standards for characterization and application of modern techniques.
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