Neurobiology Unit, Institute for Biotechnology and Biomedicine (BIOTECMED), Universitat de València, Valencia, 46100, Spain.
Spanish National Network for Research in Mental Health CIBERSAM, Madrid, 28029, Spain.
Transl Psychiatry. 2024 Oct 24;14(1):450. doi: 10.1038/s41398-024-03166-6.
The exposure to aversive experiences during early-life affects brain maturation and induces changes in behavior. Additionally, when these experiences coincide with subtle neurodevelopmental alterations, they may contribute to the emergence of psychiatric disorders, such as schizophrenia. Studies in patients and animal models have identified changes in parvalbumin (PV) expressing inhibitory neurons, highlighting their significance in the etiology of this disorder. Most studies have been focused on the cortex, but PV+ neurons also provide inhibitory input to diencephalic regions, particularly to the thalamus (through cells in the thalamic reticular nucleus, TRN) and the habenula. Remarkably, alterations in both nuclei have been described in schizophrenia. Some of these changes in PV+ cells may be mediated by perineuronal nets (PNN), specialized regions of the extracellular matrix that often surround them and regulate their synaptic input and activity. Interestingly, the physiological maturation and integration of PV+ neurons, which involves the assembly of PNN, occurs during early postnatal life. Plasticity molecules associated to inhibitory neurons, such as PSA-NCAM, or NMDA receptors (NMDAR) can also influence the structure and function of these cells. Growing evidence also indicates that glial cells regulate the physiology of PV+ neurons by influencing their maturation and modulating their synaptic connectivity. To explore the impact of early-life aversive experiences and concomitant subtle neurodevelopmental alterations on diencephalic PV+ cells, we analyzed adult male mice subjected to a double-hit model (DHM) of schizophrenia, combining a single injection of an NMDAR antagonist at P7 and post-weaning social isolation. We observed that exploratory behavior, PV+ neurons and their associated PNN, as well as PSA-NCAM and NMDAR expression and glial cells, in the TRN and the habenula were affected by the DHM or one of its factors. To our knowledge, this is the first report on such alterations in these diencephalic structures in an animal model combining neurodevelopmental alterations and early-life stress during adolescence. Our findings complement previous work on PV+ neurons in cortical regions and underscore the importance of studying diencephalic inhibitory networks and their intricate interactions with aversive experiences and neurodevelopmental alterations during early life in the context of schizophrenia.
早期生活中经历痛苦的体验会影响大脑成熟,并导致行为改变。此外,当这些经历与微妙的神经发育变化同时发生时,它们可能会导致精神疾病的出现,如精神分裂症。在患者和动物模型中的研究已经确定了表达抑制性神经元的 Parvalbumin(PV)的变化,这突出了它们在这种疾病发病机制中的重要性。大多数研究都集中在皮层上,但 PV+神经元也向间脑区域提供抑制性输入,特别是向丘脑(通过丘脑网状核中的细胞,TRN)和缰核。值得注意的是,在精神分裂症中已经描述了这两个核的改变。PV+细胞中的一些变化可能是由周围神经胶质细胞(PNN)介导的,PNN 是细胞外基质的特化区域,它们经常围绕着它们并调节它们的突触输入和活动。有趣的是,PV+神经元的生理成熟和整合,包括 PNN 的组装,发生在出生后的早期。与抑制性神经元相关的可塑性分子,如 PSA-NCAM 或 NMDA 受体(NMDAR),也可以影响这些细胞的结构和功能。越来越多的证据还表明,神经胶质细胞通过影响其成熟和调节其突触连接来调节 PV+神经元的生理学。为了探讨早期生活痛苦体验和伴随的微妙神经发育变化对间脑 PV+细胞的影响,我们分析了成年雄性小鼠在精神分裂症的双重打击模型(DHM)下的表现,该模型在 P7 时注射单一的 NMDA 拮抗剂,并在断奶后进行社交隔离。我们观察到,探索行为、TRN 和缰核中的 PV+神经元及其相关的 PNN,以及 PSA-NCAM 和 NMDAR 的表达和神经胶质细胞,受到 DHM 或其因素之一的影响。据我们所知,这是在青春期将神经发育变化和早期生活应激相结合的动物模型中首次报道这些间脑结构的改变。我们的发现补充了以前关于皮质区域中 PV+神经元的研究,并强调了在精神分裂症背景下研究间脑抑制性网络及其与痛苦体验和神经发育变化的复杂相互作用的重要性。
