Departments of Psychiatry and Pharmacology, University of Toronto, Toronto, Ontario, Canada; Centre for Addiction and Mental Health, Toronto, Ontario, Canada.
J Neurochem. 2013 Nov;127(4):552-61. doi: 10.1111/jnc.12316. Epub 2013 Jun 11.
Previously, we found decreased mitochondrial complex I subunits levels and increased protein oxidation and nitration in postmortem prefrontal cortex (PFC) from patients with bipolar disorder (BD) and schizophrenia (SCZ). The objectives of this study were to replicate our findings in an independent sample of subjects with BD, and to examine more specifically oxidative and nitrosative damage to mitochondrial and synaptosomal proteins and lipid peroxidation in myelin. We isolated mitochondria, synaptosomes, and myelin using a percoll gradient from postmortem PFC from patients with BD, SCZ, and healthy controls. Levels of mitochondrial complex I and III proteins, protein oxidation (carbonylation), and nitration (3-nitrotyrosine) were assessed using immunobloting analysis. Lipid peroxidation [lipid hydroperoxides (LPH), 8-isoprostane (8-Iso), 4-hydroxy-2-nonenal (4-HNE)] were measured using colorimetric or ELISA assays. We found decreased complex I subunits levels in BD subjects compared with control (CTL), but no difference in complex III subunits. Carbonylation was increased in synaptosomes from BD group while 3-nitrotyrosine was increased in mitochondria from BD and SCZ groups. 8-Iso was found increased in the BD group while 4-HNE was increased in both SCZ and BD when compared with controls with no differences in LPH. Our results suggest that in BD mitochondrial proteins are more susceptible to potentially reversible nitrosative damage while more longstanding oxidative damage occurs to synaptic proteins. Oxidative stress has been shown to be higher in the brain of patients with bipolar disorder (BD). Here, we demonstrated increased levels of protein oxidation in synaptosomes from postmortem prefrontal cortex from patients from BD group, while 3-nitrotyrosine was increased in mitochondria from BD and schizophrenia (SCZ) groups. Moreover, lipid peroxidation was found increased in the BD when compared with controls; suggesting that in BD mitochondrial proteins are more susceptible to potentially reversible nitrosative damage while more longstanding oxidative damage occurs to synaptic proteins.
先前,我们发现双相情感障碍 (BD) 和精神分裂症 (SCZ) 患者死后的前额叶皮质 (PFC) 中线粒体复合物 I 亚基水平降低,蛋白质氧化和硝化增加。本研究的目的是在 BD 患者的独立样本中复制我们的发现,并更具体地检查线粒体和突触体蛋白的氧化和硝化损伤以及髓鞘中的脂质过氧化。我们使用 Percoll 梯度从 BD、SCZ 和健康对照患者的死后 PFC 中分离出线粒体、突触体和髓鞘。使用免疫印迹分析评估线粒体复合物 I 和 III 蛋白、蛋白质氧化(羰基化)和硝化(3-硝基酪氨酸)的水平。使用比色或 ELISA 测定法测量脂质过氧化[脂质氢过氧化物 (LPH)、8-异前列腺素 (8-Iso)、4-羟基-2-壬烯醛 (4-HNE)]。我们发现与对照 (CTL) 相比,BD 患者的复合物 I 亚基水平降低,但复合物 III 亚基没有差异。BD 组的突触体中的羰基化增加,而 BD 和 SCZ 组的线粒体中的 3-硝基酪氨酸增加。与对照组相比,BD 组的 8-Iso 增加,而 SCZ 和 BD 组的 4-HNE 增加,但 LPH 无差异。我们的结果表明,在 BD 中,线粒体蛋白更容易受到潜在可逆的硝化损伤,而突触蛋白则发生更持久的氧化损伤。氧化应激已被证明在双相情感障碍 (BD) 患者的大脑中更高。在这里,我们发现在 BD 组的死后前额叶皮质的突触体中蛋白质氧化水平升高,而 3-硝基酪氨酸在 BD 和精神分裂症 (SCZ) 组的线粒体中增加。此外,与对照组相比,BD 中的脂质过氧化增加;表明在 BD 中,线粒体蛋白更容易受到潜在可逆的硝化损伤,而突触蛋白则发生更持久的氧化损伤。
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