Cerebellar fastigial nucleus histamine and its H2 but not H1 receptors might inhibit acetic acid-induced visceral nociception and improve motor coordination in rats: role of opioid system.

IF 0.8 4区 农林科学 Q3 ZOOLOGY Veterinary Research Forum Pub Date : 2023-01-01 Epub Date: 2023-10-15 DOI:10.30466/vrf.2023.1988302.3762
Fereshteh Anbarian, Esmaeal Tamaddonfard, Amir Erfanparast, Farhad Soltanalinejad-Taghiabad
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Abstract

The cerebellum and its deep nuclei contribute to the regulation of important functions including motor coordination and pain. Histamine modulates some functions of the fastigial nucleus (FN) such as motor coordination. In this study, by application of histamine and activation of its H1 and H2 receptors, the FN processing of visceral pain, general locomotor activity and motor coordination were targeted. The possible mechanism of action was followed by the inhibition of opioid receptors. The right and left sides of the FN were surgically implanted with guide cannulas. Immediately after an intraperitoneal injection of acetic acid (1.00 mL, 1.00%), the first writhing onset latency and the writhing number over 60 min were recorded. Open-field and rotarod tests were applied for general locomotor and motor coordination assessment, respectively. Histamine and dimaprit (H2 receptor agonist) increased first writhing onset latency, decreased the writhing number and increased falling time from the rod. These effects were prevented by ranitidine (H2 receptor antagonist) pre-treatment. Significant alterations were not observed by histamine H1 receptor agonist (2-pyridylethylamine) and antagonist (mepyramine). Naloxone, with no effect on falling time from the rod, inhibited the antinociceptive effects of histamine and dimaprit. Beam break number was not affected by the above-mentioned treatments. Based on the results, it can be suggested that histamine H2, but not H1 receptors at the FN might have had an inhibitory role on acetic acid-induced visceral pain and improved motor coordination. The antinociception, but not motor coordination might be mediated by FN opioid receptors.

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小脑顶核组胺及其H2而非H1受体可能抑制乙酸诱导的大鼠内脏伤害感受并改善运动协调:阿片系统的作用。
小脑及其深核有助于调节包括运动协调和疼痛在内的重要功能。组胺调节顶核(FN)的一些功能,如运动协调。在本研究中,通过应用组胺及其H1和H2受体的激活,靶向内脏疼痛的FN处理、一般运动活动和运动协调。可能的作用机制是抑制阿片受体。FN的右侧和左侧通过手术植入引导套管。在腹膜内注射乙酸(1.00mL,1.00%)后,立即记录第一次扭体开始潜伏期和60分钟以上的扭体次数。开放场地和旋转杆测试分别用于一般运动和运动协调性评估。组胺和二马必利(H2受体激动剂)增加了首次扭体起始潜伏期,减少了扭体次数,增加了从杆上落下的时间。雷尼替丁(H2受体拮抗剂)预处理可阻止这些作用。组胺H1受体激动剂(2-吡啶基乙胺)和拮抗剂(美吡拉明)未观察到显著变化。纳洛酮对落棒时间无影响,可抑制组胺和地马必利的镇痛作用。梁断裂数不受上述处理的影响。根据这些结果,可以认为FN处的组胺H2受体而不是H1受体可能对乙酸诱导的内脏疼痛具有抑制作用,并改善了运动协调。FN阿片受体介导的可能是镇痛感受,而不是运动协调。
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来源期刊
Veterinary Research Forum
Veterinary Research Forum Veterinary-General Veterinary
CiteScore
1.50
自引率
0.00%
发文量
0
审稿时长
8 weeks
期刊介绍: Veterinary Research Forum (VRF) is a quarterly international journal committed to publish worldwide contributions on all aspects of veterinary science and medicine, including anatomy and histology, physiology and pharmacology, anatomic and clinical pathology, parasitology, microbiology, immunology and epidemiology, food hygiene, poultry science, fish and aquaculture, anesthesia and surgery, large and small animal internal medicine, large and small animal reproduction, biotechnology and diagnostic imaging of domestic, companion and farm animals.
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