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首页> 外文期刊>BMC Psychiatry >Factors related to age at depression onset: the role of SLC6A4 methylation, sex, exposure to stressful life events and personality in a sample of inpatients suffering from major depression
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Factors related to age at depression onset: the role of SLC6A4 methylation, sex, exposure to stressful life events and personality in a sample of inpatients suffering from major depression

机译:与抑郁症年龄相关的因素:SLC6A4甲基化,性别,暴露于患有主要抑郁症的住院患者样本中的压力生活事件和人格的作用

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An early onset of depression is associated with higher chronicity and disability, more stressful life events (SLEs), higher negative emotionality as described by the primary emotion SADNESS and more severe depressive symptomatology compared to depression onset later in life. Additionally, methylation of the serotonin transporter gene (SLC6A4) is associated with SLEs and depressive symptoms. We investigated the relation of SLEs, SLC6A4 methylation in peripheral blood, the primary emotions SADNESS and SEEKING (measured by the Affective Neuroscience Personality Scales) as well as depressive symptom severity to age at depression onset in a sample of N?=?146 inpatients suffering from major depression. Depressed women showed higher SADNESS (t (91.05)?=???3.17, p?=?0.028, d?=???0.57) and higher SLC6A4 methylation (t (88.79)?=???2.95, p?=?0.02, d?=???0.55) compared to men. There were associations between SLEs, primary emotions and depression severity, which partly differed between women and men. The Akaike information criterion (AIC) indicated the selection of a model including sex, SLEs, SEEKING and SADNESS for the prediction of age at depression onset. SLC6A4 methylation was not related to depression severity, age at depression onset or SLEs in the entire group, but positively related to depression severity in women. Taken together, we provide further evidence that age at depression onset is associated with SLEs, personality and depression severity. However, we found no associations between age at onset and SLC6A4 methylation. The joint investigation of variables originating in biology, psychology and psychiatry could make an important contribution to understanding the development of depressive disorders by elucidating potential subtypes of depression.
机译:抑郁症的早期发病与更高的慢性和残疾,更紧张的生命事件(SLE),较高的阴性情绪,如主要情绪悲伤和更严重的抑郁症术相比,与生活中的抑郁发作相比,更严重的抑郁症状。另外,血清素转运蛋白基因(SLC6A4)的甲基化与SLES和抑郁症状有关。我们调查了SLES,SLC6A4甲基化在外周血中的关系,主要情绪悲伤和寻求(由情感神经科学人格尺度衡量)以及抑郁症在N的样品中抑郁症状严重程度,在N?= 146位入住病例中从重大抑郁症。抑郁的妇女表现出更高的悲伤(T(91.05)?= ??? 3.17,p?=Δ028,d?= ??? 0.57)和更高的SLC6a4甲基化(t(88.79)?= ??? 2.95,p?=与男性相比,0.02,D?= ??? 0.55)。斯莱斯,初级情绪和抑郁症之间有关联,部分妇女和男性部分不同。 Akaike信息标准(AIC)表示选择包括性行为,SLE,寻求和悲伤的模型,以便在抑郁发作时预测年龄。 SLC6A4甲基化与抑郁严重程度无关,抑郁症发生或整个群体中的SLES,但与妇女的抑郁严重程度正相关。我们一起携带了进一步的证据,即抑郁发作的年龄与Sles,人格和抑郁严重程度有关。然而,我们发现年龄在发病和SLC6A4甲基化之间没有关联。源自生物学,心理和精神病学的变量的联合调查对于了解通过阐明潜在的抑郁症患者的抑郁症的发展来对抑郁症的发展作出重要贡献。

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