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在精神分裂症中,精神运动迟缓与执行和记忆障碍、阴性和精神病症状、神经毒性免疫产物以及自然免疫球蛋白 M 对丙二醛的降低有关。

In schizophrenia, psychomotor retardation is associated with executive and memory impairments, negative and psychotic symptoms, neurotoxic immune products and lower natural IgM to malondialdehyde.

机构信息

Department of Psychiatry, Faculty of Medicine, Chulalongkorn University, Bangkok, Thailand.

Department of Psychiatry, Medical University of Plovdiv, Plovdiv, Bulgaria.

出版信息

World J Biol Psychiatry. 2020 Jun;21(5):383-401. doi: 10.1080/15622975.2019.1701203. Epub 2020 Feb 7.

DOI:10.1080/15622975.2019.1701203
PMID:32031479
Abstract

Stable-phase schizophrenia comprises two distinct entities namely Major Neuro-Cognitive Psychosis (MNP) and simple NP (SNP), which are defined by neuroimmune and neurocognitive abnormalities. This study investigates associations of psychomotor retardation (PMR), clinical and biomarker characteristics of schizophrenia. We recruited 40 healthy controls and 79 schizophrenia patients and measured IgA responses to tryptophan catabolites (TRYCATs), IgM to malondialdehyde and nitroso (NO)-cysteinyl, CCL-11, an immune activation index based on cytokine levels, and motor screening task (MOT) scores. PMR differentiated schizophrenia from controls and MNP from SNP. In addition, PMR was strongly associated with impairments in executive functions and episodic and semantic memory, psychotic, hostility, excitation, mannerism and negative (PHEMN) symptoms. Around 50% of the variance in PMR was predicted by the cumulative effects of the immune activation index, CCL-11, TRYCATs, NO-Cysteinyl and natural IgM. PRM can reliably be combined with PHEMN symptoms, memory and executive impairments into one latent vector reflecting overall severity of schizophrenia. PMR is a key psychopathological feature of schizophrenia mainly MNP. In addition, PMR may be driven by deficits in the compensatory immune-regulatory system and increased production of neurotoxic immune products, namely TRYCATs, IgM to NO-cysteinyl, and CCL-11, an endogenous cognition deteriorating chemokine.

摘要

稳定期精神分裂症包括两种不同的实体,即主要神经认知精神病(MNP)和单纯 NP(SNP),它们由神经免疫和神经认知异常定义。本研究调查了精神运动迟缓(PMR)与精神分裂症的临床和生物标志物特征之间的关联。我们招募了 40 名健康对照者和 79 名精神分裂症患者,并测量了色氨酸分解产物(TRYCATs)、丙二醛和亚硝酰(NO)-半胱氨酸的 IgM、趋化因子 11(CCL-11)、基于细胞因子水平的免疫激活指数和运动筛查任务(MOT)评分。PMR 将精神分裂症与对照组和 MNP 与 SNP 区分开来。此外,PMR 与执行功能、情景和语义记忆、精神病、敌意、兴奋、刻板和阴性(PHEMN)症状的损伤密切相关。PMR 的约 50%的变异可由免疫激活指数、CCL-11、TRYCATs、NO-Cysteinyl 和天然 IgM 的累积效应预测。PRM 可以可靠地与 PHEMN 症状、记忆和执行功能障碍相结合,形成一个反映精神分裂症总体严重程度的潜在向量。PMR 是精神分裂症的主要 MNP 的关键精神病理学特征。此外,PMR 可能是由补偿性免疫调节系统的缺陷和神经毒性免疫产物(即 TRYCATs、NO-cysteinyl 的 IgM 和 CCL-11,一种内源性认知恶化趋化因子)的产生增加驱动的。

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