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首页> 外文期刊>Neurotoxicity research >In Schizophrenia, Depression, Anxiety, and Physiosomatic Symptoms Are Strongly Related to Psychotic Symptoms and Excitation, Impairments in Episodic Memory, and Increased Production of Neurotoxic Tryptophan Catabolites: a Multivariate and Machine Learning Study
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In Schizophrenia, Depression, Anxiety, and Physiosomatic Symptoms Are Strongly Related to Psychotic Symptoms and Excitation, Impairments in Episodic Memory, and Increased Production of Neurotoxic Tryptophan Catabolites: a Multivariate and Machine Learning Study

机译:在精神分裂症,抑郁症,焦虑和物质症状中与精神病症状和刺激有关,发作性记忆障碍,增加神经毒性色氨酸的产量增加:多变量和机器学习研究

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Abstract The depression, anxiety and physiosomatic symptoms (DAPS) of schizophrenia are associated with negative symptoms and changes in tryptophan catabolite (TRYCAT) patterning. The aim of this study is to delineate the associations between DAPS and psychosis, hostility, excitation, and mannerism (PHEM) symptoms, cognitive tests as measured using the Consortium to Establish a Registry for Alzheimer’s Disease (CERAD) and IgA/IgM responses to TRYCATs. We included 40 healthy controls and 80 participants with schizophrenia. Depression and anxiety symptoms were measured with The Hamilton Depression (HAM-D) and Anxiety (HAM-A) Rating Scales, respectively. Physiosomatic symptoms were assessed with the Fibromyalgia and Chronic Fatigue Syndrome Rating Scale (FF). Negative symptoms as well as CERAD tests, including Verbal Fluency Test (VFT), Mini-Mental State Examination (MMSE), Word List Memory (WLM), and WL Delayed Recall were measured, while ratios of IgA responses to noxious/protective TRYCATs (IgA NOX_PRO) were computed. Schizophrenia symptoms consisted of two dimensions, a first comprising PHEM and negative symptoms, and a second DAPS symptoms. A large part of the variance in DAPS was explained by psychotic symptoms and WLM. Of the variance in HAM-D, 58.9% was explained by the regression on excitement, IgA NOX_PRO ratio, WLM, and VFT; 29.9% of the variance in HAM-A by psychotic symptoms and IgA NOX/PRO; and 45.5% of the variance in FF score by psychotic symptoms, IgA NOX/PRO, and WLM. Neural network modeling shows that PHEM, IgA NOX_PRO, WLM, and MMSE are the dominant variables predicting DAPS. DAPS appear to be driven by PHEM and negative symptoms coupled with impairments in episodic memory, especially false memory creation, while all symptom dimension and cognitive impairments may be driven by an increased production of noxious TRYCATs, including picolinic, quinolinic, and xanthurenic acid.
机译:摘要精神分裂症的抑郁症,焦虑和物质症状(DAPs)与色氨酸抗粘土(Tattercat)图案化的阴性症状和变化有关。本研究的目的是描绘点击性和精神病,敌意,刺激和习惯(PHEM)症状,认知试验,以使用该联盟来建立阿尔茨海默病(CERAD)和IGA / IGM对Trycats的反应的注册。我们包括40名健康控制和80名精神分裂症的参与者。用汉密尔顿抑郁(HAM-D)和焦虑(HAM-A)评级鳞片测量抑郁和焦虑症状。通过纤维肌痛和慢性疲劳综合征评定量表评估物质症状(FF)。测量阴性症状以及Cerad测试,包括言语流畅性测试(VFT),迷你精神状态检查(MMSE),单词列表存储器(WLM)和WL延迟召回召回,而IGA对有害/保护橄榄球的比率响应(计算Iga nox_pro)。精神分裂症症状由两个维度组成,首先包含PhEM和阴性症状,以及第二个点击症状。精神病症状和WLM解释了DAP中的大部分方差。在兴奋,IGA NOX_PRO比率,WLM和VFT上的回归解释了58.9%的差异。精神病症状和IGA NOx / PRO的29.9%的火腿-A差异;灵活症状,IGA Nox / Pro和WLM的FF评分差异的45.5%。神经网络建模表明,PHEM,IGA NOX_PRO,WLM和MMSE是预测数据端的主要变量。点击似乎是由phem和阴性症状的驱动,涉及剧目内存的损伤,尤其是假记忆创作,而所有症状维度和认知障碍可能由增加的有害试液体的产生,包括斯米洛林,喹啉和X硫酸。

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