精神分裂症患者血浆基质金属蛋白酶9升高与抗精神病治疗反应差和白质密度缺陷有关

IF 3 Q2 PSYCHIATRY Schizophrenia (Heidelberg, Germany) Pub Date : 2024-08-27 DOI:10.1038/s41537-024-00494-w
Xiaojing Li, Xiujuan Wang, Yongfeng Yang, Jiahui Zhou, Xufei Wu, Jingyuan Zhao, Jianhong Zhang, Xiaoge Guo, Minglong Shao, Meng Song, Xi Su, Yong Han, Qing Liu, Tengfei Chen, Luwen Zhang, Bing Liu, Weihua Yue, Luxian Lv, Wenqiang Li
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引用次数: 0

摘要

氧化应激和神经炎症是精神分裂症(SCZ)的病理因素,并可能影响治疗效果。基质金属蛋白酶9(MMP9)是介导氧化应激和炎症之间相互作用的关键分子节点,因此可能影响治疗效果。在此,我们研究了血浆 MMP9 浓度与抗精神病药物反应、临床症状和大脑结构之间的关系。本研究共纳入了129名健康对照者和124名SCZ患者。患者在接受为期8周的抗精神病药物治疗期间接受临床监测,并被分为反应差者(49人)和反应良好者(75人)。然后,我们比较了健康对照组在基线时的血浆MMP9浓度、SCZ应答组在基线时的血浆MMP9浓度以及8周抗精神病治疗方案后的血浆MMP9浓度。我们还使用 MATRICS 共识认知测验对认知功能进行了检测。此外,我们还从患者的磁共振图像中提取了区域白质密度。与健康对照组相比,基线反应差的患者血浆MMP9水平显著升高,并与右颞上回白质密度和治疗后认知症状的变化呈负相关。相反,良好反应者与健康对照组之间的血浆 MMP9 没有明显差异,良好反应者的血浆 MMP9 与认知症状或区域白质密度也没有关联。血浆MMP9升高与SCZ患者抗精神病药物疗效差和白质缺损有关,因此可能是指导个性化治疗的有用生物标志物。
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Elevated plasma matrix metalloproteinase 9 in schizophrenia patients associated with poor antipsychotic treatment response and white matter density deficits.

Oxidative stress and neuroinflammation contribute to schizophrenia (SCZ) pathology and may influence treatment efficacy. Matrix metalloproteinase 9 (MMP9) is a critical molecular node mediating the interaction between oxidative stress and inflammation, and so may influence treatment efficacy. Here we examined the associations of plasma MMP9 concentration with antipsychotic drug responses, clinical symptoms, and brain structure. A total of 129 healthy controls and 124 patients with SCZ were included in this study. Patients were monitored clinically during 8 weeks of antipsychotic treatment and classified as poor responders (n = 49) or good responders (n = 75). We then compared plasma MMP9 concentrations in healthy controls at baseline and both SCZ responder groups at baseline and after the 8-week antipsychotic treatment regimen. Cognitive function was also examined using the MATRICS Consensus Cognitive Battery. In addition, we extracted regional white matter density from magnetic resonance images of patients. Compared to healthy controls, plasma MMP9 levels were significantly elevated in poor responders at baseline and negatively correlated with both white matter density in the right superior temporal gyrus and the change in cognitive symptoms after treatment. Conversely, there was no significant difference in plasma MMP9 between good responders and healthy controls, and no associations of plasma MMP9 with cognitive symptoms or regional white matter density among good responders. Elevated plasma MMP9 is associated with poor antipsychotic drug efficacy and white matter deficits in SCZ patients, and so may be a useful biomarker to guide personalized treatment.

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