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[预测双相情感障碍:我们能从前瞻性队列研究中学到什么?]

[Predicting bipolar disorder: what can we learn from prospective cohort studies?].

作者信息

Geoffroy P A, Leboyer M, Scott J

机构信息

Inserm, U955, service de psychiatrie génétique, 94000 Créteil, France; Pôle de psychiatrie (Pr Leboyer), centre expert bipolaire, hôpital Henri-Mondor - Albert-Chenevier, AP-HP, 40, rue de Mesly, 94000 Créteil cedex, France; Pôle de psychiatrie, université Lille Nord de France, CHRU de Lille, 59000 Lille, France; Fondation FondaMental, 94000 Créteil, France.

Inserm, U955, service de psychiatrie génétique, 94000 Créteil, France; Faculté de médecine, université Paris Est, 94000 Créteil, France; Pôle de psychiatrie (Pr Leboyer), centre expert bipolaire, hôpital Henri-Mondor - Albert-Chenevier, AP-HP, 40, rue de Mesly, 94000 Créteil cedex, France; Fondation FondaMental, 94000 Créteil, France.

出版信息

Encephale. 2015 Feb;41(1):10-6. doi: 10.1016/j.encep.2013.05.004. Epub 2013 Oct 3.

Abstract

INTRODUCTION

Bipolar disorder (BD) is a life course illness; and there is increasing awareness of the many personal, social and economic consequences of the illness in older adults. However, it is important to emphasize that BD usually begins in late adolescence or early adulthood and 75 % cases have a first episode in this age period. This early onset and the associated level of disability mean that BD is the 4th leading cause of global disease burden in adolescents and young adults. Internationally, mental health services are increasingly striving to diagnose and treat BD as early as possible to try to prevent poor outcomes. In addition, researchers are using methods employed previously in psychosis studies as these may help us to recognise the earliest manifestations of BD. If it is possible to identify sub-threshold and 'ultra high risk' syndromes for BD, this might lead to new interventions that could target the prevention of first episodes of mania. One approach to understanding these risk syndromes is to examine prospective community cohort studies and BD offspring studies.

METHODS

This paper reviews prospective cohort studies that identify robust risk factors in early illness onset, which was defined as age at onset of BD between 15-25 years.

RESULTS

We found that although > 50 % of individuals who developed BD had developed a putative BD prodrome prior to 14 years of age, this usually began with non-specific symptoms that overlap with similar presentations for those who later develop psychosis or severe depression. However, there are some features that seem to better identify groups with a BD "at-risk" syndrome. This syndrome is frequently composed of several factors such as mood lability, depressive episodes, prior anxiety, sleep and/or conduct disorders, attention and concentration impairment, altered energy patterns, and a family history of mania and/or depression. The course of these early predictors suggests the precursor syndromes are composed of mini-clusters of symptoms many of which are episodic and change over time. During the early phases of BD, most of the affective disturbances reported were depressive in polarity and started during adolescence, there were few manic or mixed or psychotic episodes with an onset before puberty. The pathogenesis of BD demonstrates a gradual progression from non-specific to more specific symptoms and then to frank BD features.

CONCLUSION

Prospective community and offspring BD cohort studies are approaches that together can help us understand the evolution of BD and allow us to define the developmental pathways. Further, identifying subjects with BD "at-risk" syndrome using a clinical staging model may allow benign interventions to be used as first-line treatment - such as neuroprotective agents like essential fatty acids; second line treatments, with a less benign risk to benefit ratio should be reserved for severe or resistant cases.

摘要

引言

双相情感障碍(BD)是一种贯穿一生的疾病;人们越来越意识到该疾病对老年人在个人、社会和经济方面造成的诸多后果。然而,必须强调的是,BD通常始于青春期后期或成年早期,75%的病例在这个年龄段首次发病。这种早发情况及相关的残疾程度意味着BD是青少年和青年全球疾病负担的第四大主要原因。在国际上,心理健康服务机构越来越努力尽早诊断和治疗BD,以试图预防不良后果。此外,研究人员正在采用先前在精神病研究中使用的方法,因为这些方法可能有助于我们识别BD的最早表现。如果能够识别BD的亚阈值和“超高风险”综合征,这可能会带来针对预防躁狂首次发作的新干预措施。理解这些风险综合征的一种方法是研究前瞻性社区队列研究和BD后代研究。

方法

本文回顾了前瞻性队列研究,这些研究确定了疾病早发的可靠风险因素,早发定义为BD发病年龄在15至25岁之间。

结果

我们发现,虽然超过50%患BD的个体在14岁之前就已出现假定的BD前驱症状,但这些症状通常始于非特异性症状,与后来患精神病或重度抑郁症者的类似表现重叠。然而,有一些特征似乎能更好地识别具有BD“风险”综合征的群体。这种综合征通常由几个因素组成,如情绪不稳定、抑郁发作、既往焦虑、睡眠和/或行为障碍、注意力和专注力受损、能量模式改变以及躁狂和/或抑郁家族史。这些早期预测因素的病程表明,前驱综合征由症状小集群组成,其中许多是发作性的且随时间变化。在BD的早期阶段,报告的大多数情感障碍在极性上为抑郁,始于青春期,青春期前很少有躁狂、混合或精神病性发作。BD的发病机制显示出从非特异性症状逐渐发展为更特异性症状,然后发展为明显的BD特征的过程。

结论

前瞻性社区和BD后代队列研究共同有助于我们理解BD的演变,并使我们能够定义其发展途径。此外,使用临床分期模型识别具有BD“风险”综合征的受试者,可能会使良性干预措施用作一线治疗——如必需脂肪酸等神经保护剂;二线治疗的风险收益比不太理想,应保留用于严重或难治性病例。

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