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自杀行为中血清素能系统的遗传学

Genetics of the serotonergic system in suicidal behavior.

作者信息

Arango Victoria, Huang Yung-yu, Underwood Mark D, Mann J John

机构信息

Department of Neuroscience, New York State Psychiatric Institute, New York, NY 10032, USA.

出版信息

J Psychiatr Res. 2003 Sep-Oct;37(5):375-86. doi: 10.1016/s0022-3956(03)00048-7.

DOI:10.1016/s0022-3956(03)00048-7
PMID:12849930
Abstract

Genetic factors contribute to the risk of psychopathology in many psychiatric conditions, but the specific genes are yet to be identified. Neurotransmitter alterations are implicated in the etiology of psychopathology based, in part, on studies of neurotransmitter receptors and their biosynthetic or degradative enzymes in postmortem tissue. Identification of the altered receptors and enzymes serves to identify candidate genes of potential etiological significance. Polymorphisms in these genes can contribute to alterations in protein function in vivo that are part of the neurochemical underpinnings of psychopathologies such as major depressive disorder, psychoses, alcoholism, personality disorders, aggressive-impulsive traits, or suicidal behavior. Altered serotonergic function is implicated in the etiology and pathogenesis of several major psychiatric conditions. In particular, there is much evidence for an association of lower serotonergic function and suicidal behavior. Thus genes related to the serotonergic system are candidate genes worthy of study as part of the genetic diathesis for suicidal behavior. This review examines the following polymorphisms in the serotonin biosynthetic enzyme tryptophan hydroxylase (TPH; A779C substitution), the serotonin transporter (5-HTT, 5-HTTLPR allele), the 5-HT(1B) receptor (G861C, C129T substitution) and the 5-HT(2A) receptor (T102C) for their relationship to suicidal behavior. For the TPH gene, we found the less common U or A allele variant of the A779C polymorphism was associated with suicide attempt. Other studies have found the U allele to be associated with aggression and lower serotonergic function in vivo. A 44 base pair insertion/deletion in the 5' flanking promoter region of the 5-HTT gene may result in less 5-HTT expression and 5-HTT binding. We examined 220 cases postmortem and found no association between the promoter genotype and 5-HTT binding. We also found no association with major depressive disorder (MDD), suicide or pathological aggression, despite finding significantly fewer 5-HTT sites in the prefrontal cortex of depressed and/or suicide cases. In genomic DNA samples from 178 unrelated subjects, we detected two polymorphisms for the 5-HT(1B) receptor at nucleotides 861 and 129. However, no association between either polymorphism and depression, suicide, aggression, or alcoholism was observed. There are two common polymorphisms for the 5-HT(2A) receptor gene in humans. The results of studies of 5-HT(2A) receptor gene polymorphisms do not indicate significant major associations with suicidal behavior. In contrast, the 5-HT(2A) receptor itself is reported to be increased in suicide. Functional polymorphisms involving the promoter region that affect gene expression may explain this finding. Studies of candidate genes related to serotonergic function in brain are increasingly used to establish genetic alterations contributing to psychiatric illness. The most meaningful studies combine the study of candidate genes with direct measures of related proteins as well as psychopathology.

摘要

遗传因素在许多精神疾病中都与精神病理学风险相关,但具体基因尚未确定。神经递质改变与精神病理学的病因有关,部分基于对死后组织中神经递质受体及其生物合成或降解酶的研究。确定改变的受体和酶有助于识别具有潜在病因学意义的候选基因。这些基因中的多态性可导致体内蛋白质功能改变,而这是诸如重度抑郁症、精神病、酗酒、人格障碍、攻击冲动特质或自杀行为等精神病理学神经化学基础的一部分。血清素能功能改变与几种主要精神疾病的病因和发病机制有关。特别是,有大量证据表明血清素能功能降低与自杀行为有关。因此,与血清素能系统相关的基因是作为自杀行为遗传素质一部分值得研究的候选基因。本综述研究了血清素生物合成酶色氨酸羟化酶(TPH;A779C替换)、血清素转运体(5-HTT,5-HTTLPR等位基因)、5-HT(1B)受体(G861C、C129T替换)和5-HT(2A)受体(T102C)的以下多态性与自杀行为的关系。对于TPH基因,我们发现A779C多态性中较不常见的U或A等位基因变体与自杀未遂有关。其他研究发现U等位基因与攻击行为以及体内较低的血清素能功能有关。5-HTT基因5'侧翼启动子区域的44个碱基对插入/缺失可能导致5-HTT表达和5-HTT结合减少。我们对220例死后病例进行了检查,发现启动子基因型与5-HTT结合之间没有关联。我们还发现与重度抑郁症(MDD)、自杀或病理性攻击行为无关,尽管在抑郁和/或自杀病例的前额叶皮质中发现5-HTT位点明显较少。在来自178名无关受试者的基因组DNA样本中,我们在核苷酸861和129处检测到5-HT(1B)受体的两种多态性。然而,未观察到任何一种多态性与抑郁症自杀、攻击行为或酗酒之间的关联。人类5-HT(2A)受体基因有两种常见的多态性。5-HT(2A)受体基因多态性的研究结果并未表明与自杀行为有显著的主要关联。相比之下,据报道5-HT(2A)受体本身在自杀中会增加。涉及影响基因表达的启动子区域的功能性多态性可能解释了这一发现。对与大脑血清素能功能相关的候选基因的研究越来越多地用于确定导致精神疾病的基因改变。最有意义的研究将候选基因的研究与相关蛋白质的直接测量以及精神病理学结合起来。

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