Palomo Tomás, Kostrzewa Richard M., Archer Trevor, Beninger Richard J.
Servicio Psiquiátrico, Hospital Universitario 12 de Octubre, Avda. de Córdoba s/n, 28041 Madrid, Spain.
Neurotox Res. 2002 Aug-Sep;4(5-6):397-408. doi: 10.1080/1029842021000022061.
There is now considerable evidence that both schizophrenia and affective disorders have their origin at least in part in events that occur during early pre- and post-natal development. In the case of schizophrenia, many observations, for example, increased risk for schizophrenia in the offspring of mothers who had influenza A during their second trimester of pregnancy and evidence for abnormal neuronal migration in the cerebral cortex of post mortem tissue from schizophrenic patients, suggest that a second trimester insult may have occurred and that this insult may have increased the risk for the development of schizophrenia in late adolescence or early adulthood. Animal studies have found that rats that undergo exocitotoxic damage to the ventral hippocampus on postnatal day 7 develop exaggerated sensitivity to dopamine-stimulating drugs or to stressful stimuli that becomes apparent after sexual maturity but not before, providing a neurodevelopmental model of schizophrenia. Similarly, post-weaning social isolation leads to enhanced responses to dopaminergic drugs and to stress that emerges after sexual maturity. These animal models are proving to be valuable tools to study the neurobiological mechanisms mediating the influence of early insults to the nervous system on later behavioural functions. In the case of affective disorders, although the evidence is not as strong, a number of the same observations have been made suggesting that an insult during early ontogeny may lead to the development of affective disorders later in life. For example, retrospective studies of people with affective disorders showed that they were more likely to have attained motor milestones at a later age and to have had poorer academic performance as children. There is a wealth of evidence suggesting hyperfunctioning of the hypothalamic-pituitary-adrenal (HPA) axis in affective disorders. Animal studies have shown that early maternal deprivation can lead to lasting changes in the reactivity of the HPA axis to stressful stimuli, providing another link from early experience to adult psychopathology. Continued studies of the effects of pre- and early post-natal events on the development of the nervous system and the relationships of these events to schizophrenia or affective disorder will provide new insights into the mechanisms underlying these common neuropsychiatric illnesses.
现在有大量证据表明,精神分裂症和情感障碍至少部分起源于出生前和出生后早期发育过程中发生的事件。就精神分裂症而言,许多观察结果表明,例如,在怀孕中期感染甲型流感的母亲所生的后代患精神分裂症的风险增加,以及对精神分裂症患者死后组织大脑皮质中神经元迁移异常的证据,表明可能在怀孕中期发生了一次损伤,并且这种损伤可能增加了在青春期后期或成年早期患精神分裂症的风险。动物研究发现,出生后第7天腹侧海马体遭受外毒素损伤的大鼠,对多巴胺刺激药物或应激刺激表现出过度敏感,这种敏感在性成熟后才会显现出来,而在性成熟前则不会,这提供了一个精神分裂症的神经发育模型。同样,断奶后的社会隔离会导致对多巴胺能药物和应激的反应增强,这种反应在性成熟后出现。这些动物模型被证明是研究介导早期神经系统损伤对后期行为功能影响的神经生物学机制的有价值工具。就情感障碍而言,尽管证据没有那么确凿,但也有一些相同的观察结果表明,个体发育早期的一次损伤可能导致晚年情感障碍的发生。例如,对情感障碍患者的回顾性研究表明,他们在较晚年龄才达到运动发育里程碑,并且在儿童时期学业成绩较差。有大量证据表明情感障碍患者下丘脑 - 垂体 - 肾上腺(HPA)轴功能亢进。动物研究表明,早期母体剥夺可导致HPA轴对应激刺激的反应性发生持久变化,这提供了另一条从早期经历到成人精神病理学的联系。对出生前和出生后早期事件对神经系统发育的影响以及这些事件与精神分裂症或情感障碍的关系的持续研究,将为这些常见神经精神疾病的潜在机制提供新的见解。
