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[双相情感障碍、抑郁症和精神分裂症中对氧磷酶Q192R的表型变异]

[Phenotypic Variants of Paraoxonase Q192R in Bipolar Disorder,Depression and Schizophrenia].

作者信息

Atagün Murat İlhan, Tunç Serhat, Alışık Murat, Erel Özcan

出版信息

Turk Psikiyatri Derg. 2018 Summer;29(2):79-86.

PMID:30215835
Abstract

OBJECTIVE

Activity of the paraoxonase 1 (PON1) enzyme varies prominently according to the PON1 Q192R genotype. The arginine (R) genotype hydrolyzes peroxided lipids more quickly and efficiently than the glutamine (Q) genotype. The Q phenotype suggests greater liability to neurodegenerative processes, cardiovascular and malignancy risks than the R phenotype. Stimulated PON/ARES ratio is associated with the PON1 Q192R polymorphism. This study aimes to assess the Q192R phenotype in schizophrenia, bipolar disorder and depression.

METHOD

Patients with schizophrenia (37), bipolar disorder (n=50), depression (n=43) and healthy volunteers (n=43) were enrolled. Serum PON1, stimulated paraoxonase (sPON) and aryl esterase (ARES) levels were assessed with an automatic analyzer. Clusters of sPON/ARES ratio were detected with frequency analysis in PON1. QQ, QR and RR variant groups.

RESULTS

There were significant differences between the bipolar disorder, depression, schizophrenia and healthy volunteer groups in terms of phenotype frequencies in groups (Fisher's Exact Coefficient=18.96, p=0.003). A higher prevalence of the PON1 RR variant was found in bipolar disorder whereas the PON1 QQ variant had a higher prevalence in depression and schizophrenia as compared to others. Serum PON1 activity correlated with number of episodes in the bipolar disorder group and with SANS, SAPS scores in the schizophrenia group.

CONCLUSION

Difference between bipolar disorder, schizophrenia and depression in PON1 activity and PON1 phenotype might be suggestive of different liability to lipid peroxidation and neurodegeneration between the diagnostic groups. Longitudinal studies may identify long term differences between PON1 Q192R polymorphisms in clinical outcomes and neuropathology.

摘要

目的

对氧磷酶1(PON1)的活性根据PON1 Q192R基因型有显著差异。精氨酸(R)基因型比谷氨酰胺(Q)基因型能更快、更有效地水解过氧化脂质。与R表型相比,Q表型提示更易发生神经退行性病变、心血管疾病和恶性肿瘤风险。刺激后的PON/ARES比值与PON1 Q192R多态性相关。本研究旨在评估精神分裂症、双相情感障碍和抑郁症患者的Q192R表型。

方法

纳入精神分裂症患者(37例)、双相情感障碍患者(n = 50)、抑郁症患者(n = 43)和健康志愿者(n = 43)。用自动分析仪检测血清PON1、刺激对氧磷酶(sPON)和芳基酯酶(ARES)水平。通过频率分析在PON1 QQ、QR和RR变异组中检测sPON/ARES比值聚类情况。

结果

双相情感障碍组、抑郁症组、精神分裂症组和健康志愿者组在表型频率方面存在显著差异(Fisher精确系数 = 18.96,p = 0.003)。双相情感障碍组中PON1 RR变异的患病率较高,而与其他组相比,抑郁症和精神分裂症组中PON1 QQ变异的患病率较高。双相情感障碍组血清PON1活性与发作次数相关,精神分裂症组与阴性症状评定量表(SANS)、阳性症状评定量表(SAPS)评分相关。

结论

双相情感障碍、精神分裂症和抑郁症在PON1活性和PON1表型上的差异可能提示不同诊断组之间脂质过氧化和神经退行性变的易感性不同。纵向研究可能会发现PON1 Q192R多态性在临床结局和神经病理学方面的长期差异。

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