抑郁症的定量精神病理学:纽卡斯尔量表的应用

Acta psychiatrica Belgica Pub Date : 1994-01-01
L Staner
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引用次数: 0

摘要

下丘脑-垂体轴紊乱,如地塞米松(DXM)给药后血浆皮质醇逃逸或TSH对TRH的反应减弱,以及睡眠结构异常,如快速眼动潜伏期缩短,在抑郁症中经常遇到。这些异常只发生在抑郁症患者的一个亚组中,因此可以确定抑郁症的生物学或内源性成分。对于这种内源性抑郁,人们提出了几种定义。在这方面,使用生物学标准,纽卡斯尔量表仍然是最有效的临床定义。在本研究中,93例患者(女性58例,男性35例),年龄15-79岁(平均42岁),在药物洗脱期至少10天后入院进行生物调查(ddxm和TRH测试,睡眠脑电图记录)。用纽卡斯尔量表对患者进行评估,并使用SADS诊断为RDC。在控制了年龄、性别和疾病严重程度的影响后,多元回归分析显示,纽卡斯尔量表的抑郁性运动活动和体重减轻是解释神经内分泌测试结果差异的最重要的两个项目。此外,根据这两个项目的存在对样本进行二分类时,两组受试者在DXM后皮质醇值、TRH后TSH值和REM潜伏期值存在显著差异。然后使用15种内源性抑郁症的操作定义中更频繁引用的16种抑郁症状对两组(生物和非生物)进行特征描述。logistic回归分析显示,体重减轻、快感缺乏、早醒和早晨情绪恶化是生物学组与非生物学组最明显的4个症状。这些症状可能反映了抑郁症的生物学异常,是内源性抑郁症的核心。
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[Quantitative psychopathology of depression: application of the Newcastle Scale].

Hypothalamo-pituitary axis disturbances, such as plasma cortisol escape after dexamethasone (DXM) administration or blunted TSH response to TRH, and sleep architecture abnormalities such as shortened REM latency are frequently encountered in depressive disorders. These anomalies only occur in a subgroup of depressed patients and could thus identify a biological or endogenous component to depressive illness. Several definitions of this endogenous depression have been proposed. In this regard, using biological criteria, the Newcastle scale remains the strongest validated clinical definition. In this study, 93 patients (58 women and 35 men) aged 15-79 years (mean: 42) who complained about a depressed mood were admitted for biological investigations (DXM and TRH tests, sleep EEG recording) after a drug wash-out period of at least 10 days. Patients were assessed with the Newcastle scale and diagnosed with RDC using the SADS. After the effects of age, gender and severity of illness were controlled for, multiple regression analyses showed that depressive pychomotor activity and weight loss were the 2 items of the Newcastle scale most contributing to explain the variances of the neuroendocrine tests results. Moreover, when the sample was dichotomized according to the presence of these 2 items, the 2 groups had significantly different post DXM cortisol values, TSH levels after TRH and REM latency values. The 2 groups (biological and non-biological) were then characterized using 16 depressive symptoms more frequently cited in 15 operational definitions of endogenous depression. A logistic regression analysis showed that weight loss, anhedonia, early awakening, and morning worsening of mood were the 4 symptoms that best distinguished biological from non-biological patients group. These symptoms could reflect biological abnormalities in depression and form the core of the endogenous depression.

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