（+）-TAN-67对小鼠中痛敏肽/孤啡肽抗伤害感受作用的调节效应。

Kamei J, Ohsawa M, Suzuki T, Saitoh A, Endoh T, Narita M, Tseng L F, Nagase H

Department of Pathophysiology and Therapeutics, Faculty of Pharmaceutical Sciences, Hoshi University, 4-41, Ebara 2-chome, Shinagawa-ku, Tokyo, Japan.

Eur J Pharmacol. 1999 Nov 3;383(3):241-7. doi: 10.1016/s0014-2999(99)00648-2.

To clarify the pharmacological properties of (+)2-Methyl-4aalpha-(3-hydroxyphenyl)-1, 2, 3, 4, 4a, 5, 12, 12aalpha-octahydro-quinolino[2, 3, 3-g]isoquinoline ((+)-TAN-67), the effect of (+)-TAN-67 on the antinociception induced by the intrathecal (i.t.) administration of nociceptin/orphanin FQ was studied in mice using the tail-flick test and the formalin test. I.t. administration of (+)-TAN-67, at doses of 1 to 10 ng, facilitated the tail-flick response in a dose-dependent manner in mice. In addition, i.t. administration of (+)-TAN-67 (1 to 10 ng) in mice produced a marked pain-like aversive responses. I.t. pretreatment with D-Pro(9)-[spiro-gamma-lactam]-Leu(10)-Trp(11)-physalaemin(1-11) (GR82334, 0.1-1.0 nmol), a potent and selective tachykinin NK(1) receptor antagonist, dose-dependently blocked the reduction of the tail-flick response induced by (+)-TAN-67. Furthermore, (+)-TAN-67-induced facilitation of the tail-flick response was abolished in capsaicin-treated mice. On the other hand, (+)-TAN-67-induced flinching responses were dose-dependently and significantly reduced by i.t. pretreatment with GR82334 (0.1-1.0 nmol). The duration of i.t. (+)-TAN-67-induced flinching responses was significantly reduced in capsaicin-treated mice as compared with naive mice. I.t. administration of nociceptin/orphanin FQ (1-10 nmol) dose-dependently increased the tail-flick latency. I.t. administration of nociceptin/orphanin FQ (0.1-1.0 nmol) significantly and dose-dependently reduced the first-phase nociceptive response, but not the second-phase nociceptive response. I.t. pretreatment with (+)-TAN-67 (0.3-3.0 microg) for 30 min dose-dependently attenuated the antinociception induced by i.t. nociceptin (10 nmol) in the tail-flick test. Furthermore, the antinociceptive effect of nociceptin/orphanin FQ (1 nmol, i.t.) on the first-phase response in the formalin test was dose-dependently attenuated by s.c. pretreatment with (+)-TAN-67 (0.3-3.0 microg). (+)-TAN-67 (0.3-3.0 microg, i.t.), by itself, did not facilitate the tail-flick response or produce apparent behavioral changes. It is possible that (+)-TAN-67 has an antagonistic effect on nociceptin/orphanin FQ-induced antinociception.

为阐明(+)-2-甲基-4aα-(3-羟基苯基)-1,2,3,4,4a,5,12,12aα-八氢喹啉并[2,3,3-g]异喹啉((+)-TAN-67)的药理特性，采用甩尾试验和福尔马林试验，在小鼠中研究了(+)-TAN-67对鞘内(i.t.)注射孤啡肽/孤啡肽FQ诱导的抗伤害感受的影响。以1至10 ng的剂量i.t.注射(+)-TAN-67，可使小鼠的甩尾反应呈剂量依赖性增强。此外，在小鼠中i.t.注射(+)-TAN-67(1至10 ng)会产生明显的类似疼痛的厌恶反应。用强效且选择性的速激肽NK(1)受体拮抗剂D-脯氨酸(9)-[螺-γ-内酰胺]-亮氨酸(10)-色氨酸(11)-雨蛙肽(1-11)(GR82334，0.1 - 1.0 nmol)进行i.t.预处理，可剂量依赖性地阻断(+)-TAN-67诱导的甩尾反应减弱。此外，在辣椒素处理的小鼠中，(+)-TAN-67诱导的甩尾反应增强被消除。另一方面，用GR82334(0.1 - 1.0 nmol)进行i.t.预处理可剂量依赖性且显著地降低(+)-TAN-67诱导的退缩反应。与未处理的小鼠相比，辣椒素处理的小鼠中i.t.注射(+)-TAN-67诱导的退缩反应持续时间显著缩短。i.t.注射孤啡肽/孤啡肽FQ(1 - 10 nmol)可使甩尾潜伏期呈剂量依赖性延长。i.t.注射孤啡肽/孤啡肽FQ(0.1 - 1.0 nmol)可显著且剂量依赖性地降低第一阶段伤害性反应，但不影响第二阶段伤害性反应。在甩尾试验中，用(+)-TAN-67(0.3 - 3.0 μg)进行i.t.预处理30分钟，可剂量依赖性地减弱i.t.注射孤啡肽(10 nmol)诱导的抗伤害感受。此外，在福尔马林试验中，用(+)-TAN-67(0.3 - 3.0 μg)进行皮下预处理可剂量依赖性地减弱孤啡肽/孤啡肽FQ(1 nmol，i.t.)对第一阶段反应的抗伤害感受作用。(+)-TAN-67(0.3 - 3.0 μg，i.t.)本身不会增强甩尾反应或产生明显的行为变化。(+)-TAN-67可能对孤啡肽/孤啡肽FQ诱导的抗伤害感受具有拮抗作用。