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氯胺酮诱导的精神分裂症啮齿动物模型中脑源性神经营养因子(BDNF)的变化:一项系统综述

Brain-derived neurotrophic factor (BDNF) changes in rodent models of schizophrenia induced by ketamine: a systematic review.

作者信息

Motamedi-Manesh Atefeh, Asanjan Mahdieh Farzin, Fallah Hamed, Gharibian Shahrzad, Taghavi Alireza, Poode Zahra Haghighi, Akhondzadeh Shahin, Vaseghi Salar

机构信息

Cognitive Neuroscience Lab, Medicinal Plants Research Center, Institute of Medicinal Plants, ACECR, Karaj, Iran.

Middle East Technical University, Ankara, Türkiye.

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 2025 Feb 20. doi: 10.1007/s00210-025-03912-7.

Abstract

Schizophrenia is a severe neuropsychiatric disorder ranking among the top ten global disability causes. In rodents, sub-chronic or chronic ketamine treatment is used for the induction of schizophrenia. Ketamine affects the function of brain-derived neurotrophic factor (BDNF), the most important neurotrophin involved in the pathophysiology of different neuropsychiatric disorders. The present systematic review aimed to investigate BDNF changes in rodent studies used ketamine-induced schizophrenia. PubMed electronic database was searched and 44 articles were found. After removal of unrelated articles, 17 articles were selected. The results showed a wide range of inconsistent changes in BDNF levels. We found that sub-chronic and chronic ketamine treatment in rats decreased BDNF or had no effect. Sub-chronic and chronic ketamine treatment in mice only decreased BDNF. However, increased BDNF was commonly observed following acute ketamine treatment. These results showed the possible role of species and the duration of treatment. Also, sex can also be involved in BDNF changes because one study showed inconsistent BDNF changes in male and female rats. In conclusion, we found that ketamine's effects may depend on factors such as duration of administration, sex, and species. Therefore, the wide range of BDNF changes may be related to high variability in methods. Because of this variability, there is currently no standardized method for using ketamine as a rodent model for schizophrenia. Further research is needed to establish a standardized pharmacological model of schizophrenia using ketamine treatment.

摘要

精神分裂症是一种严重的神经精神障碍,在全球十大致残原因中名列前茅。在啮齿动物中,使用亚慢性或慢性氯胺酮治疗来诱导精神分裂症。氯胺酮会影响脑源性神经营养因子(BDNF)的功能,BDNF是参与不同神经精神障碍病理生理学的最重要的神经营养因子。本系统综述旨在调查在使用氯胺酮诱导精神分裂症的啮齿动物研究中BDNF的变化。检索了PubMed电子数据库,共找到44篇文章。剔除无关文章后,选取了17篇文章。结果显示BDNF水平存在广泛的不一致变化。我们发现,对大鼠进行亚慢性和慢性氯胺酮治疗会降低BDNF水平或无影响。对小鼠进行亚慢性和慢性氯胺酮治疗只会降低BDNF水平。然而,急性氯胺酮治疗后通常会观察到BDNF水平升高。这些结果表明了物种和治疗持续时间可能起到的作用。此外,性别也可能参与BDNF的变化,因为一项研究表明雄性和雌性大鼠的BDNF变化不一致。总之,我们发现氯胺酮的作用可能取决于给药持续时间、性别和物种等因素。因此,BDNF变化范围广泛可能与方法的高度变异性有关。由于这种变异性,目前尚无将氯胺酮用作精神分裂症啮齿动物模型的标准化方法。需要进一步研究以建立使用氯胺酮治疗的精神分裂症标准化药理模型。

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