Serum levels of oxidants and protein S100B were associated in the first-episode drug naïve patients with schizophrenia

L. Lei, Yanli Li, Yun Bian, Fude Yang, Xianyun Li, Xiaole Han, Li Tian, Song Chen, Zhiren Wang, Yunlong Tan
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Abstract

Background: Patients with schizophrenia have been noted with an elevation of serum S100B protein concentration, but the pathological process is not known. This study was to investigate the relationship between levels of S100B protein and oxidative stress. Methods: General information and blood sample were collected from the first-episode drug naïve or drug-free acute stage of patients who met the Diagnostic and Statistical Manual of Mental Disorders-IV (DSM-IV) criteria for schizophrenia and healthy controls. The serum levels of S100B, total oxidants (TOS) and malonaldehyde (MDA) were used to measure the level of oxidative stress in both patients, and healthy controls. General linear regression analysis was performed to examine the association of S100B protein with the levels of oxidative stress. Results: The levels of serum protein S100B were associated with the concentration of both TOS (Beta=15.77; p=0.0038) and MDA (Beta=7.90; p=0.0068) in the first-episode drug-naive patients (n=29).While both associations were no longer significant (p>0.05) in the drug-free acute phase patients (n=29); the levels of serum S100B was still consistently associated with TOS (Beta=12.42;p=0.0026) and MDA(Beta=4.11;p=0.0480) in the combined group of patients group(n=58). Simultaneous analysis of both oxidative markers, we still found that both TOS (Beta=12.88; p=0.0103) and MDA (Beta=6.46; p=0.0167) were associated with the serum level of protein S100B in the first-episode drug-naive patients, but not drug-free acute phase patients. Conclusion: Our results suggest that astrocyte activity, serum levels of oxidants, and their cross-talking might be involved in the pathogenesis of schizophrenia. This warrants a further study for understanding the underlying mechanism.
精神分裂症首发药物naïve患者血清中氧化剂和蛋白S100B水平相关
背景:精神分裂症患者血清S100B蛋白浓度升高,但病理过程尚不清楚。本研究旨在探讨S100B蛋白水平与氧化应激的关系。方法:收集符合精神障碍诊断与统计手册- iv (DSM-IV)精神分裂症标准的首发药物naïve或无药物急性期患者的一般资料和血样。用血清S100B、总氧化剂(TOS)和丙二醛(MDA)水平测定两组患者和健康对照组的氧化应激水平。采用一般线性回归分析来检验S100B蛋白与氧化应激水平的关系。结果:血清蛋白S100B水平与两种TOS浓度相关(Beta=15.77;p=0.0038)和MDA (Beta=7.90;P =0.0068) (n=29)。而在无药物急性期患者(n=29),两种相关性不再显著(p>0.05);联合用药组(n=58)血清S100B水平与TOS (Beta=12.42, p=0.0026)和MDA(Beta=4.11, p=0.0480)仍然一致相关。同时分析两种氧化标志物,我们仍然发现两者的TOS (Beta=12.88;p=0.0103)和MDA (Beta=6.46;p=0.0167)与首次用药患者血清S100B蛋白水平相关,但与无药急性期患者无关。结论:星形胶质细胞活性、血清氧化剂水平及其相互作用可能参与了精神分裂症的发病机制。这需要进一步的研究来了解潜在的机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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