预处理血清MCP-1水平预测精神分裂症患者对利培酮的反应。

Yezhe Lin, Yanmin Peng, Cuizhen Zhu, Yousong Su, Yuan Shi, Zhiguang Lin, Jinghong Chen, Donghong Cui
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引用次数: 7

摘要

背景:精神分裂症是一种慢性衰弱性疾病。其发病机制和治疗可能与炎性细胞因子有关。很少有研究集中在预测细胞因子对抗精神病药物的反应。目的:探讨细胞因子是否能预测抗精神病药物的疗效。方法:采用横断面和自然观察队列研究:(1)比较精神分裂症患者(n=64)和健康对照组(n=53)血清IL-1β、TNF-α和MCP-1的基线水平;(2)探讨基线细胞因子对奥氮平和利培酮单药治疗后精神病理的影响。结果:(1)精神分裂症患者MCP-1基线水平显著高于健康对照组(t=2.62, p=0.010), IL-1β (t=1.43, p=0.154)和TNF-α (t=0.79, p=0.434)差异无统计学意义;(2)利培酮单药治疗4周后,MCP-1预处理水平与PANSS-G降低显著相关(r =-0.658;页= 0.855);(3)进一步逐步多元线性回归分析表明,治疗前较高的MCP-1水平是利培酮单药治疗后精神分裂症患者PANSS-G降低的显著预测因子(校正R2= 0.409, β = -0.658, p)。结论:MCP-1可能在精神分裂症发病机制中发挥作用。预处理MCP-1水平可作为利培酮治疗反应的生物标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Pretreatment Serum MCP-1 Level Predicts Response to Risperidone in Schizophrenia.

Pretreatment Serum MCP-1 Level Predicts Response to Risperidone in Schizophrenia.

Pretreatment Serum MCP-1 Level Predicts Response to Risperidone in Schizophrenia.

Background: Schizophrenia is a chronic debilitating disease. The pathogenesis and treatment may be associated with inflammatory cytokines. There are few studies focusing on the prediction of cytokines in response to antipsychotics.

Aim: To investigate whether cytokines would predict response to antipsychotics.

Methods: Cross-sectional and natural observational cohort studies were applied to:(1) compare the baseline levels of serum IL-1β, TNF-α and MCP-1 between schizophrenia (n=64) and healthy controls (n=53); (2) To investigate the impact of baseline cytokines to psychopathology following olanzapine and risperidone monotherapy.

Results: (1) Baseline MCP-1 level of patients with schizophrenia was significantly higher than healthy controls (t=2.62, p=0.010), while no significance was found in IL-1β (t=1.43, p=0.154) and TNF-α (t=0.79, p=0.434); (2) Pretreatment level of MCP-1 significantly correlated with PANSS-G reduction following 4 weeks' of risperidone monotherapy (r =-0.658; p<0.001) but not olanzapine monotherapy (r =-0.031; p=0.855); (3) Further stepwise multiple linear regression analysis indicated that higher MCP-1 level prior to treatment was a significant predictor of less PANSS-G reduction in schizophrenia patients following risperidone monotherapy (adjusted R2= 0.409, β = -0.658, p <0.001), but not in the olanzapine group.

Conclusion: MCP-1 may play a role in the pathogenesis of schizophrenia. Pretreatment level of MCP-1 may serve as a biomarker indicating response to risperidone treatment.

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