速激肽NK1受体拮抗剂CP-99,994在清醒沙鼠中的抗伤害感受活性

Antinociceptive activity of the tachykinin NK1 receptor antagonist, CP-99,994, in conscious gerbils.

作者信息

Rupniak N M, Webb J K, Williams A R, Carlson E, Boyce S, Hill R G

机构信息

Merck Sharp and Dohme Research Laboratories, Neuroscience Research Centre, Terlings Park, Harlow, Essex.

出版信息

Br J Pharmacol. 1995 Sep;116(2):1937-43. doi: 10.1111/j.1476-5381.1995.tb16686.x.

DOI:10.1111/j.1476-5381.1995.tb16686.x

PMID:8528583

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1909089/

Abstract

The ability of CP-99,994, and its less active enantiomer, CP-100,263, to inhibit spontaneous behaviours and hyperalgesia induced by central infusion of the NK1 receptor agonist, GR73632 or intraplantar injection of formalin was investigated in rats and gerbils. 2. GR73632 (3 pmol, i.c.v.)-induced foot tapping in gerbils was dose-dependently inhibited by CP-99,994 (0.1-1 mg kg-1, s.c.), but not by CP-100,263 (10 mg kg-1, s.c.) using pretreatment times up to 60 min. The centrally active dose-range for CP-99,994 was increased to 1-10 mg kg-1 s.c. with a higher challenge dose of GR73632 (30 pmol, i.c.v.). 3. In gerbils, intrathecal (i.t.) injection of GR73632 (30 pmol) elicited behaviours (licking, foot tapping or flinching and face washing) which closely resembled, but which was less specifically localized than, behaviours seen in animals injected with formalin (0.1-5%) into one hindpaw. 4. In rats, CP-100,263, but not CP-99,994 (up to 30 mg kg-1), inhibited the early phase response to intraplantar injection of 5% formalin (ID50 = 13.9 mg kg-1). The late phase was inhibited by both compounds (ID50 values 36.3 and 20.9 mg kg-1, respectively). In gerbils, there was marginal evidence for enantioselective inhibition of the early phase induced by formalin (2%). The ID50 values were 6.2 mg kg-1 for CP-99,994 and 13.4 mg kg-1 for CP-100,263. 5. Intrathecal injection of GR73632 (30 pmol) caused thermal hyperalgesia in igerbils which was inhibited enantioselectively by s.c. administration of CP-99,994 (ID50= 2.46 mg kg-1), but not by CP-100,263 (30 mg kg-1).6. In gerbils, intraplantar injection of formalin (0.1%) caused thermal hyperalgesia which was inhibited by CP-99,994 (ID50= 1.1 mg kg-1, s.c.). There was a nonsignificant trend for an anti-algesic effect of CP-100,236 (estimated ID50 = 8.2 mg kg-1, s.c.).7 These findings support the proposal that NK1 receptor antagonists may be useful in the clinical management of pain and reinforce the need to dissociate specific and nonspecific antinociceptive effects of available compounds.

摘要

研究了CP - 99,994及其活性较低的对映体CP - 100,263在大鼠和沙鼠中抑制由中枢注射NK1受体激动剂GR73632或足底注射福尔马林诱导的自发行为和痛觉过敏的能力。2. 沙鼠中，GR73632（3 pmol，脑室内注射）诱导的足部轻敲行为，在预处理时间长达60分钟时，CP - 99,994（0.1 - 1 mg kg-1，皮下注射）呈剂量依赖性抑制，但CP - 100,263（10 mg kg-1，皮下注射）无此作用。当GR73632的激发剂量更高（30 pmol，脑室内注射）时，CP - 99,994的中枢活性剂量范围增加至1 - 10 mg kg-1皮下注射。3. 在沙鼠中，鞘内注射GR73632（30 pmol）引发的行为（舔舐、足部轻敲或退缩以及洗脸）与向一只后爪注射福尔马林（0.1 - 5%）的动物所表现的行为相似，但定位特异性较低。4. 在大鼠中，CP - 100,263可抑制足底注射5%福尔马林的早期反应（ID50 = 13.9 mg kg-1），而CP - 99,994（高达30 mg kg-1）则无此作用。两种化合物均可抑制晚期反应（ID50值分别为36.3和20.9 mg kg-1）。在沙鼠中，有少量证据表明对福尔马林（2%）诱导的早期反应存在对映体选择性抑制。CP - 99,994的ID50值为6.2 mg kg-1，CP - 100,263的ID50值为13.4 mg kg-1。5. 鞘内注射GR73632（30 pmol）在沙鼠中引起热痛觉过敏，皮下注射CP - 99,994（ID50 = 2.46 mg kg-1）可对映体选择性抑制该反应，但CP - 100,263（未注明剂量）则无此作用。6. 在沙鼠中，足底注射福尔马林（0.1%）引起热痛觉过敏，CP - 99,994（ID50 = 1.1 mg kg-1，皮下注射）可抑制该反应。CP - 100,236有非显著性的镇痛作用趋势（估计ID50 = 8.2 mg kg-1，皮下注射）。7. 这些发现支持了NK1受体拮抗剂可能在疼痛临床治疗中有用的观点，并强化了区分现有化合物特异性和非特异性抗伤害感受作用的必要性。