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5-羟色胺3(5-HT3)受体拮抗剂阿洛司琼在躯体和内脏痛觉过敏大鼠模型中的作用。

Effects of the 5-HT3 receptor antagonist, alosetron, in a rat model of somatic and visceral hyperalgesia.

作者信息

Miranda Adrian, Peles Shachar, McLean Peter G, Sengupta Jyoti N

机构信息

Department of Pediatrics, Medical College of Wisconsin, Milwaukee, WI, USA.

出版信息

Pain. 2006 Dec 15;126(1-3):54-63. doi: 10.1016/j.pain.2006.06.014. Epub 2006 Jul 17.

DOI:10.1016/j.pain.2006.06.014
PMID:16844296
Abstract

Conflicting results exist regarding the role of 5-HT3 receptors in somatic and visceral nociceptive processing. We aimed to investigate the effects of the 5-HT3 receptor antagonist, alosetron, in a rat model of somatic and visceral hyperalgesia. Two injections (100 microl) of either pH 4.0 or 7.2 saline were given unilaterally in the gastrocnemius (GN) muscle. In all groups, the paw withdrawal thresholds (PWT) to von Frey filaments and the visceromotor responses (VMR) to colorectal distension (CRD) were recorded before the saline injections and 72 h, and 1 week after the second injection. Intrathecal (i.t.) (25 nmol) or intravenous (i.v.) (100 microg/kg/day) alosetron was given daily following the second injection and compared to either i.v. or i.t. saline (vehicle). There was a significant decrease in the mean PWT bilaterally in all groups following pH 4.0 injections (p<0.05). Intravenous alosetron resulted in a significant increase in the PWT bilaterally on days 2 and 3. Intrathecal alosetron resulted in significant increase in the PWT starting at day 3 and was significantly higher than baseline on days 4-7 (p<0.05). At CRD pressures 30 mmHg, the VMR of pH 4.0 injected rats was significantly increased at 72 h and 1 week (p<0.05). Both i.v. and i.t. alosetron treated rats failed to demonstrate any alteration in the VMR. Control rats (pH 7.2) failed to show any alteration in the VMR and were unaffected by alosetron. Both, systemically and centrally administered alosetron, reversed the mechanical somatic hypersensitivity and prevented the development of visceral hyperalgesia, suggesting a centrally mediated effect.

摘要

关于5-羟色胺3(5-HT3)受体在躯体和内脏伤害性信息处理中的作用,存在相互矛盾的结果。我们旨在研究5-HT3受体拮抗剂阿洛司琼在大鼠躯体和内脏痛觉过敏模型中的作用。在腓肠肌(GN)单侧注射两剂(100微升)pH 4.0或7.2的生理盐水。在所有组中,在注射生理盐水前、第二次注射后72小时和1周记录对von Frey细丝的爪部撤离阈值(PWT)以及对结肠扩张(CRD)的内脏运动反应(VMR)。第二次注射后每天鞘内注射(i.t.)(25纳摩尔)或静脉注射(i.v.)(100微克/千克/天)阿洛司琼,并与静脉注射或鞘内注射生理盐水(赋形剂)进行比较。在注射pH 4.0后,所有组双侧的平均PWT均显著降低(p<0.05)。静脉注射阿洛司琼导致在第2天和第3天双侧PWT显著增加。鞘内注射阿洛司琼从第3天开始导致PWT显著增加,并且在第4 - 7天显著高于基线(p<0.05)。在CRD压力为30毫米汞柱时,注射pH 4.0的大鼠的VMR在72小时和1周时显著增加(p<0.05)。静脉注射和鞘内注射阿洛司琼治疗的大鼠在VMR方面均未表现出任何改变。对照大鼠(pH 7.2)在VMR方面未表现出任何改变,并且不受阿洛司琼影响。全身和中枢给予阿洛司琼均可逆转机械性躯体超敏反应并预防内脏痛觉过敏的发生,提示存在中枢介导的效应。

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