6-羟多巴胺治疗喹匹罗强迫症大鼠的行为改变及其多巴胺能强迫循环机制

IF 2.5 4区 医学 Q3 NEUROSCIENCES
Haowen Zheng, Rui He, Yang Ming, Haiping He, Wei Wang, Ligang Chen, Feilong Gong
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引用次数: 0

摘要

背景:最近的研究表明,内囊前肢可能是多个强迫回路的汇聚区域。本研究通过6-羟多巴胺(6-OHDA)选择性损伤相应靶点的多巴胺能神经元或纤维,描绘位于内囊前肢的各种强迫环的解剖图谱,探讨不同多巴胺能强迫环在强迫症(OCD)机制中的作用。方法:选取52只雄性SD大鼠,每周2次给予生理盐水(1 mL/kg, NS组,n = 6)或喹匹罗(QNP,多巴胺d2激动剂,0.5 mg/kg, n = 46),连续5周。每次注射后,大鼠被放置在一个开放的场地上,以分析它们的行为方面,包括访问大本营的次数(NOH),每次访问大本营的平均时间(ATBO)和总旅行距离(TDM)。造模后,将46只QNP大鼠随机分为5组:6- ohda内膜前肢(AC)立体定向注射组(QNP+AC组,n = 10)、6- ohda丘脑中背核(MD)立体定向注射组(QNP+MD组,n = 10)、6- ohda伏隔核(NAC)立体定向注射组(QNP+NAC组,n = 10)、生理盐水立体定向注射组(QNP+NS- s组,n = 10)、非手术组(QNP+Non-S组,n = 6)。NS组大鼠同时接受6- ohda立体定向注射(NS+6- ohda -s组,n = 6);Ac2, md2, nac2)各组大鼠继续给予QNP,每周2次,连续4周,每次输注后观察其行为。4周后,采用免疫荧光染色法监测干预神经环不同区域多巴胺神经元和神经纤维的分布,并进行定量分析。结果:QNP+AC组和QNP+NAC组患者的强迫行为在术后3周和4周逐渐下降,其中QNP+AC组下降更快。QNP+MD组在术后3周下降,但在术后4周上升至与术前几乎相同的水平。术后荧光染色和定量分析显示,与QNP+Non-S组相比,6-OHDA注射相应靶区多巴胺(DA)神经元或神经纤维数量明显减少。结论:6-羟多巴胺选择性损伤强迫症回路内多巴胺能神经元或神经纤维靶点,在一定程度上缓解强迫症行为。结果表明,AC可能是强迫症治疗干预的最佳靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Behavior Changes in Quinpirole Obsessive-Compulsive Disorder Rats Treated with 6-Hydroxydopamine and the Corresponding Dopaminergic Compulsive Loop Mechanism.

Background: Recent studies suggest that the anterior limb of the internal capsule may be an area of convergence for multiple compulsion loops. In this study, the role of different dopaminergic compulsion loops in the mechanism of obsessive-compulsive disorder (OCD) was investigated by selectively damaging dopaminergic neurons or fibers in the corresponding targets with 6-hydroxydopamine (6-OHDA) and depicting the anatomical map of various compulsion loops located in the anterior limb of the internal capsule.

Methods: A total of 52 male Sprague Dawley (SD) rats were exposed to either saline (1 mL/kg, NS group, n = 6) or quinpirole (QNP, dopamine D2-agonist, 0.5 mg/kg, n = 46) twice weekly for 5 weeks. After each injection, the rats were placed on an open field to analyze aspects of their behaviour, including the number of home base visits (NOH), average time between each home base visit (ATBO), and total distance travelled (TDM). After model setup, 46 QNP rats were divided randomly into five groups: 6-OHDA anterior limb of internal capsule (AC) stereotactic injection group (QNP+AC group, n = 10), 6-OHDA mediodorsal thalamic nucleus (MD) stereotactic injection group (QNP+MD group, n = 10), 6-OHDA nucleus accumbens (NAC) stereotactic injection group (QNP+NAC group, n = 10), saline stereotactic injection group (QNP+NS-S group, n = 10), and non-surgical group (QNP+Non-S group, n = 6). In the NS group, rats simultaneously received a 6-OHDA stereotactic injection (NS+6-OHDA-S group, n = 6: AC2, MD2, NAC2). All QNP-treated rats were then continued to be given QNP twice a week for 4 weeks, and their behaviour was observed after each infusion. After 4 weeks, immunofluorescence staining was used to monitor the distribution of dopamine neurons and nerve fibers in different areas of the intervention nerve loops, and quantitative analysis was performed.

Results: Compulsive behaviour declined gradually in the QNP+AC and QNP+NAC groups 3 and 4 weeks after surgery, with the QNP+AC group decreasing more rapidly. The QNP+MD group had decreased by 3 weeks after surgery but increased to almost the same level as pre-surgery at 4 weeks post-surgery. Postoperative fluorescence staining and quantitative analysis suggested the number of dopamine (DA) neurons or nerve fibers in the corresponding target area of the 6-OHDA injection were significantly reduced compared with the QNP+Non-S group.

Conclusions: 6-OHDA selectively damages the targets of dopaminergic neurons or nerve fibers within the OCD loop, which somewhat alleviates compulsive behaviours. The results suggest that the AC might be the best target for therapeutic interventions for OCD.

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来源期刊
CiteScore
2.80
自引率
5.60%
发文量
173
审稿时长
2 months
期刊介绍: JIN is an international peer-reviewed, open access journal. JIN publishes leading-edge research at the interface of theoretical and experimental neuroscience, focusing across hierarchical levels of brain organization to better understand how diverse functions are integrated. We encourage submissions from scientists of all specialties that relate to brain functioning.
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