The Contribution of Adult Hippocampal Neurogenesis to the Progression of Psychiatric Disorders.

Modern trends in pharmacopsychiatry Pub Date : 2017-01-01 Epub Date: 2017-07-24 DOI:10.1159/000470812
Rachel A Kohman, Justin S Rhodes
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引用次数: 16

Abstract

New neurons are continuously formed in the adult hippocampus of the human, nonhuman primate, and rodent throughout life though rates of neurogenesis precipitously decline with age to near zero levels at the end of the natural life span. Since its discovery in the 1960s, a large number of studies have documented numerous environmental and genetic factors which regulate adult neurogenesis. Chief among the positive regulators of neurogenesis are exercise and antidepressant drugs. Chief among the negative regulators of neurogenesis besides age are stress and inflammation. To the extent that many psychiatric disorders are comorbid with or causally related to stress and inflammation, decreased neurogenesis could be a partial contributor to the pathophysiology of the disorders. However, the functional significance of new neurons in behavior has yet to be established and is currently a hotly debated topic. Therefore, it is not clear whether changes in neurogenesis that occur alongside psychiatric illnesses are a cause or a consequence of the mediating factors such as stress, drug abuse, and inflammation, which are complexly involved in the disorders. It will be important moving forward to use modern technologies capable of instantaneously inactivating cohorts of new neurons to test their functional significance in behavior and the etiology of mental illnesses.

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成人海马神经发生对精神疾病进展的贡献。
在人类、非人类灵长类动物和啮齿动物的成年海马体中,新的神经元在一生中不断形成,尽管神经发生率随着年龄的增长而急剧下降,在自然寿命结束时接近于零水平。自20世纪60年代发现以来,大量的研究记录了许多调节成人神经发生的环境和遗传因素。运动和抗抑郁药物是神经发生的主要积极调节因素。除年龄外,神经发生的主要负调节因子是压力和炎症。在某种程度上,许多精神疾病与压力和炎症共病或有因果关系,神经发生减少可能是疾病病理生理学的部分原因。然而,新神经元在行为中的功能意义尚未确定,目前是一个激烈争论的话题。因此,目前尚不清楚伴随精神疾病发生的神经发生变化是压力、药物滥用和炎症等介导因素的原因还是结果,这些因素与精神疾病复杂相关。这将是重要的向前迈进,使用现代技术能够即时灭活的新神经元群,以测试其功能意义的行为和精神疾病的病因。
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Inflammation Effects on Glutamate as a Pathway to Neuroprogression in Mood Disorders. The Link between Refractoriness and Neuroprogression in Treatment-Resistant Bipolar Disorder. The Contribution of Adult Hippocampal Neurogenesis to the Progression of Psychiatric Disorders. Neurodegeneration, Neuroregeneration, and Neuroprotection in Psychiatric Disorders. Pharmacological and Nonpharmacological Interventions to Arrest Neuroprogression in Psychiatric Disorders.
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