Department of Molecular Biology, University of Bergen, PB 7803, N-5020 Bergen, Norway.
Aquat Toxicol. 2011 Oct;105(3-4):206-17. doi: 10.1016/j.aquatox.2011.06.010. Epub 2011 Jun 15.
Polychlorinated biphenyls (PCBs) are still widespread environmental pollutants that bioaccumulate and biomagnify in the aquatic food chains despite the ban on their production. They constitute a class of 209 possible congeners with different chlorination pattern of the biphenyl ring structure resulting in many different toxicities and mechanisms of toxicity. The neurotoxicity of PCBs is relatively poorly understood, and biomarkers for their neurotoxic effects are lacking. We have carried out a proteomic analysis of brain tissue from Atlantic cod (Gadus morhua) exposed to 2,2',4,4',5,5'-hexachlorobiphenyl (PCB 153, ortho-substituted and non-coplanar), a previously demonstrated neurotoxic congener and the most prevalent congener in biological samples. The fish received 0, 0.5, 2 and 8 mg/kg PCB 153 by intraperitoneal injection, half of the dose on the first day and the second half after one week, and were exposed for two weeks in total. Using a 2-DE approach we found 56 protein spots to be 20% or more (≤ 0.8-fold or ≥ 1.2-fold) significantly different between at least one of the three PCB 153-exposed groups and the control group, and 27 of these were identified by MALDI-TOF MS and MS/MS. Approximately 80% of the differentially regulated proteins may be associated with a non stressor-specific response and/or have previously been classified as notoriously differentially regulated in 2-DE/MS based proteomics studies, such as alterations/responses in energy metabolism, cytoskeleton, protein synthesis, protein degradation (ubiquitin-proteasome system), cellular growth, cycle and death (14-3-3 protein), and (surprisingly) axon guidance (dihydropyrimidinase-like 2 (=collapsin response mediator protein 2, CRMP-2)). The six remaining affected proteins include the strongest up-regulated protein, pyridoxal kinase (essential for synthesis of neurotransmitters such as dopamine, serotonin and GABA), nicotinamide phosphoribosyl-transferase (involved in protection against axonal degeneration) and protein phosphatase 1 (controls brain recovery by synaptic plasticity). The last three of these six proteins (deltex, Rab14 and sorting nexin 6) may preliminarily identify involvement of the Notch signaling pathway and endosomal function in PCB 153-induced neurotoxicity. Our findings constitute novel clues for further research on PCB 153 mode of action in brain, and a proper selection of proteins may, following validation, be applicable in a panel of biomarkers for aquatic environmental monitoring.
多氯联苯 (PCBs) 是仍然广泛存在的环境污染物,尽管已禁止其生产,但它们仍在水生食物链中生物累积和生物放大。它们由 209 种可能的同系物组成,其联苯环结构的氯化模式不同,导致许多不同的毒性和毒性机制。PCBs 的神经毒性相对了解较少,并且缺乏其神经毒性作用的生物标志物。我们对暴露于 2,2',4,4',5,5'-六氯联苯 (PCB 153,邻位取代且非共平面) 的大西洋鳕鱼 (Gadus morhua) 的脑组织进行了蛋白质组学分析,PCB 153 是一种先前证明的神经毒性同系物,也是生物样本中最普遍的同系物。鱼通过腹腔注射接受 0、0.5、2 和 8 mg/kg PCB 153,第一天一半,一周后另一半,总共暴露两周。使用 2-DE 方法,我们发现至少有三个 PCB 153 暴露组中的一个与对照组相比,有 56 个蛋白质斑点的差异在 20%或更多(≤ 0.8 倍或≥ 1.2 倍),其中 27 个通过 MALDI-TOF MS 和 MS/MS 鉴定。大约 80%的差异调节蛋白可能与非应激特异性反应相关,或者以前被归类为基于 2-DE/MS 的蛋白质组学研究中明显差异调节的蛋白,例如能量代谢、细胞骨架、蛋白质合成、蛋白质降解(泛素-蛋白酶体系统)、细胞生长、周期和死亡(14-3-3 蛋白)和(令人惊讶的是)轴突导向(二氢嘧啶酶样 2(= collapsin 反应介质蛋白 2,CRMP-2))。其余六个受影响的蛋白质包括上调最强烈的蛋白质,吡哆醛激酶(合成神经递质如多巴胺、血清素和 GABA 所必需)、烟酰胺磷酸核糖转移酶(参与保护轴突退化)和蛋白磷酸酶 1(通过突触可塑性控制大脑恢复)。这六个中的最后三个蛋白质(deltex、Rab14 和分选连接蛋白 6)可能初步确定 Notch 信号通路和内体功能参与 PCB 153 诱导的神经毒性。我们的研究结果为进一步研究 PCB 153 在大脑中的作用模式提供了新的线索,并且经过验证后,适当选择的蛋白质可能适用于水生环境监测的生物标志物组。
