{"title":"Alzheimer's disease as a synaptopathy: Evidence for dysfunction of synapses during disease progression.","authors":"Soraya Meftah, Jian Gan","doi":"10.3389/fnsyn.2023.1129036","DOIUrl":null,"url":null,"abstract":"<p><p>The synapse has consistently been considered a vulnerable and critical target within Alzheimer's disease, and synapse loss is, to date, one of the main biological correlates of cognitive decline within Alzheimer's disease. This occurs prior to neuronal loss with ample evidence that synaptic dysfunction precedes this, in support of the idea that synaptic failure is a crucial stage within disease pathogenesis. The two main pathological hallmarks of Alzheimer's disease, abnormal aggregates of amyloid or tau proteins, have had demonstrable effects on synaptic physiology in animal and cellular models of Alzheimer's disease. There is also growing evidence that these two proteins may have a synergistic effect on neurophysiological dysfunction. Here, we review some of the main findings of synaptic alterations in Alzheimer's disease, and what we know from Alzheimer's disease animal and cellular models. First, we briefly summarize some of the human evidence to suggest that synapses are altered, including how this relates to network activity. Subsequently, animal and cellular models of Alzheimer's disease are considered, highlighting mouse models of amyloid and tau pathology and the role these proteins may play in synaptic dysfunction, either in isolation or examining how the two pathologies may interact in dysfunction. This specifically focuses on neurophysiological function and dysfunction observed within these animal models, typically measured using electrophysiology or calcium imaging. Following synaptic dysfunction and loss, it would be impossible to imagine that this would not alter oscillatory activity within the brain. Therefore, this review also discusses how this may underpin some of the aberrant oscillatory patterns seen in animal models of Alzheimer's disease and human patients. Finally, an overview of some key directions and considerations in the field of synaptic dysfunction in Alzheimer's disease is covered. This includes current therapeutics that are targeted specifically at synaptic dysfunction, but also methods that modulate activity to rescue aberrant oscillatory patterns. Other important future avenues of note in this field include the role of non-neuronal cell types such as astrocytes and microglia, and mechanisms of dysfunction independent of amyloid and tau in Alzheimer's disease. The synapse will certainly continue to be an important target within Alzheimer's disease for the foreseeable future.</p>","PeriodicalId":12650,"journal":{"name":"Frontiers in Synaptic Neuroscience","volume":null,"pages":null},"PeriodicalIF":2.8000,"publicationDate":"2023-03-09","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10033629/pdf/","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Frontiers in Synaptic Neuroscience","FirstCategoryId":"3","ListUrlMain":"https://doi.org/10.3389/fnsyn.2023.1129036","RegionNum":4,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"2023/1/1 0:00:00","PubModel":"eCollection","JCR":"Q2","JCRName":"NEUROSCIENCES","Score":null,"Total":0}
引用次数: 0
Abstract
The synapse has consistently been considered a vulnerable and critical target within Alzheimer's disease, and synapse loss is, to date, one of the main biological correlates of cognitive decline within Alzheimer's disease. This occurs prior to neuronal loss with ample evidence that synaptic dysfunction precedes this, in support of the idea that synaptic failure is a crucial stage within disease pathogenesis. The two main pathological hallmarks of Alzheimer's disease, abnormal aggregates of amyloid or tau proteins, have had demonstrable effects on synaptic physiology in animal and cellular models of Alzheimer's disease. There is also growing evidence that these two proteins may have a synergistic effect on neurophysiological dysfunction. Here, we review some of the main findings of synaptic alterations in Alzheimer's disease, and what we know from Alzheimer's disease animal and cellular models. First, we briefly summarize some of the human evidence to suggest that synapses are altered, including how this relates to network activity. Subsequently, animal and cellular models of Alzheimer's disease are considered, highlighting mouse models of amyloid and tau pathology and the role these proteins may play in synaptic dysfunction, either in isolation or examining how the two pathologies may interact in dysfunction. This specifically focuses on neurophysiological function and dysfunction observed within these animal models, typically measured using electrophysiology or calcium imaging. Following synaptic dysfunction and loss, it would be impossible to imagine that this would not alter oscillatory activity within the brain. Therefore, this review also discusses how this may underpin some of the aberrant oscillatory patterns seen in animal models of Alzheimer's disease and human patients. Finally, an overview of some key directions and considerations in the field of synaptic dysfunction in Alzheimer's disease is covered. This includes current therapeutics that are targeted specifically at synaptic dysfunction, but also methods that modulate activity to rescue aberrant oscillatory patterns. Other important future avenues of note in this field include the role of non-neuronal cell types such as astrocytes and microglia, and mechanisms of dysfunction independent of amyloid and tau in Alzheimer's disease. The synapse will certainly continue to be an important target within Alzheimer's disease for the foreseeable future.
突触一直被认为是阿尔茨海默病中一个脆弱而关键的靶点,迄今为止,突触丧失是阿尔茨海默病认知能力下降的主要生物学相关因素之一。这发生在神经元丧失之前,有大量证据表明突触功能障碍发生在神经元丧失之前,这支持了突触衰竭是疾病发病机制中关键阶段的观点。阿尔茨海默病的两个主要病理标志--淀粉样蛋白或 tau 蛋白的异常聚集,在阿尔茨海默病的动物和细胞模型中对突触生理产生了明显的影响。此外,越来越多的证据表明,这两种蛋白可能会对神经生理功能紊乱产生协同作用。在此,我们将回顾阿尔茨海默病突触改变的一些主要发现,以及我们从阿尔茨海默病动物模型和细胞模型中了解到的情况。首先,我们简要总结了一些人类证据,这些证据表明突触发生了改变,包括突触与网络活动的关系。随后,我们考虑了阿尔茨海默病的动物和细胞模型,重点介绍了淀粉样蛋白和 tau 病理学小鼠模型,以及这些蛋白在突触功能障碍中可能发挥的作用,无论是单独作用还是研究这两种病理学如何在功能障碍中相互作用。这特别侧重于在这些动物模型中观察到的神经生理功能和功能障碍,通常使用电生理学或钙成像技术进行测量。在突触功能障碍和丧失之后,不可能想象这不会改变大脑内的振荡活动。因此,本综述还讨论了这可能是阿尔茨海默病动物模型和人类患者中某些异常振荡模式的基础。最后,综述了阿尔茨海默病突触功能障碍领域的一些关键方向和注意事项。这包括目前专门针对突触功能障碍的治疗方法,以及调节活动以挽救异常振荡模式的方法。该领域未来值得关注的其他重要方向包括非神经元细胞类型(如星形胶质细胞和小胶质细胞)的作用,以及阿尔茨海默病中独立于淀粉样蛋白和 tau 的功能障碍机制。在可预见的未来,突触必将继续成为阿尔茨海默病的一个重要靶点。