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喹硫平对源自大鼠后代的器官型皮质培养物中小胶质细胞轨迹和炎症反应潜在影响的见解。

Insights into the Potential Impact of Quetiapine on the Microglial Trajectory and Inflammatory Response in Organotypic Cortical Cultures Derived from Rat Offspring.

作者信息

Chamera Katarzyna, Curzytek Katarzyna, Kamińska Kinga, Trojan Ewa, Leśkiewicz Monika, Tylek Kinga, Regulska Magdalena, Basta-Kaim Agnieszka

机构信息

Laboratory of Immunoendocrinology, Department of Experimental Neuroendocrinology, Maj Institute of Pharmacology, Polish Academy of Sciences, 12 Smętna St., 31-343 Kraków, Poland.

出版信息

Biomedicines. 2023 May 9;11(5):1405. doi: 10.3390/biomedicines11051405.

DOI:10.3390/biomedicines11051405
PMID:37239076
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10216789/
Abstract

Atypical antipsychotics currently constitute the first-line medication for schizophrenia, with quetiapine being one of the most commonly prescribed representatives of the group. Along with its specific affinity for multiple receptors, this compound exerts other biological characteristics, among which anti-inflammatory effects are strongly suggested. Simultaneously, published data indicated that inflammation and microglial activation could be diminished by stimulation of the CD200 receptor (CD200R), which takes place by binding to its ligand (CD200) or soluble CD200 fusion protein (CD200Fc). Therefore, in the present study, we sought to evaluate whether quetiapine could affect certain aspects of microglial activity, including the CD200-CD200R and CX3CL1-CX3CR1 axes, which are involved in the regulation of neuron-microglia interactions, as well as the expression of selected markers of the pro- and anti-inflammatory profile of microglia (, , , , , , and ). Concurrently, we examined the impact of quetiapine and CD200Fc on the IL-6 and IL-10 protein levels. The abovementioned aspects were investigated in organotypic cortical cultures (OCCs) prepared from the offspring of control rats (control OCCs) or those subjected to maternal immune activation (MIA OCCs), which is a widely implemented approach to explore schizophrenia-like disturbances in animals. The experiments were performed under basal conditions and after additional exposure to the bacterial endotoxin lipopolysaccharide (LPS), according to the "two-hit" hypothesis of schizophrenia. The results of our research revealed differences between control and MIA OCCs under basal conditions and in response to treatment with LPS in terms of lactate dehydrogenase and nitric oxide release as well as , , and expression. The additional stimulation with the bacterial endotoxin resulted in a notable change in the mRNA levels of pro- and anti-inflammatory microglial markers in both types of OCCs. Quetiapine diminished the influence of LPS on , , and expression in control OCCs as well as on IL-6 and IL-10 levels in MIA OCCs. Moreover, CD200Fc reduced the impact of the bacterial endotoxin on IL-6 production in MIA OCCs. Thus, our results demonstrated that quetiapine, as well as the stimulation of CD200R by CD200Fc, beneficially affected LPS-induced neuroimmunological changes, including microglia-related activation.

摘要

非典型抗精神病药物目前是精神分裂症的一线用药,喹硫平是该类药物中最常被处方的代表药物之一。除了对多种受体具有特异性亲和力外,这种化合物还具有其他生物学特性,其中强烈提示具有抗炎作用。同时,已发表的数据表明,通过刺激CD200受体(CD200R)可以减轻炎症和小胶质细胞活化,这是通过其与配体(CD200)或可溶性CD200融合蛋白(CD200Fc)结合来实现的。因此,在本研究中,我们试图评估喹硫平是否会影响小胶质细胞活性的某些方面,包括参与调节神经元-小胶质细胞相互作用的CD200-CD200R和CX3CL1-CX3CR1轴,以及小胶质细胞促炎和抗炎特征的选定标志物的表达(,,,,,,和)。同时,我们研究了喹硫平和CD200Fc对IL-6和IL-10蛋白水平的影响。上述方面在由对照大鼠后代制备的器官型皮质培养物(OCCs)(对照OCCs)或经历母体免疫激活(MIA OCCs)的培养物中进行研究,这是一种在动物中广泛用于探索精神分裂症样障碍的方法。根据精神分裂症的“双打击”假说,实验在基础条件下以及额外暴露于细菌内毒素脂多糖(LPS)后进行。我们的研究结果揭示了在基础条件下以及对LPS治疗的反应中,对照OCCs和MIA OCCs在乳酸脱氢酶和一氧化氮释放以及,,和表达方面存在差异。细菌内毒素的额外刺激导致两种类型的OCCs中促炎和抗炎小胶质细胞标志物的mRNA水平发生显著变化。喹硫平减弱了LPS对对照OCCs中,,和表达的影响以及对MIA OCCs中IL-6和IL-10水平的影响。此外,CD200Fc降低了细菌内毒素对MIA OCCs中IL-6产生的影响。因此,我们的结果表明,喹硫平以及CD200Fc对CD200R 的刺激有益地影响了LPS诱导的神经免疫变化,包括与小胶质细胞相关的活化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/583c/10216789/f61c41520d3c/biomedicines-11-01405-g001.jpg
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Naunyn Schmiedebergs Arch Pharmacol. 2023 Jul;396(7):1423-1433. doi: 10.1007/s00210-023-02406-8. Epub 2023 Feb 3.
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Basic Clin Neurosci. 2022 May-Jun;13(3):335-347. doi: 10.32598/bcn.2021.3361.1. Epub 2022 May 1.
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