Amann R, Schuligoi R, Holzer P, Donnerer J
Institut für experimentelle und klinische Pharmakologie, Universität Graz, Austria.
Naunyn Schmiedebergs Arch Pharmacol. 1995 Aug;352(2):201-5. doi: 10.1007/BF00176775.
In anaesthetized rats, the neurokinin (NK)1 receptor antagonist SR140333 (10-1000 micrograms/kg) stereo-selectively inhibited mustard oil-induced plasma protein extravasation in the dorsal skin of the hind paw. After s.c. administration of SR140333, inhibition of plasma protein extravasation was maximal 3 h after injection. A dose of 0.1 mg/kg i.v. or 1.0 mg/kg s.c. produced long-lasting inhibition which was still significant 24 h after treatment. Since systemic administration of SR140333 has been shown to inhibit nociceptive responses in anaesthetized rats, we wanted to evaluate a possible effect of SR140333 on chemo- and thermonociception in conscious rats. SR140333 (100 micrograms/kg s.c.) did not reduce the behavioral response of rats to the irritant effect of capsaicin in the wiping test, nor did it affect the thermal nociceptive threshold in the plantar test. Furthermore, the decrease in thermal nociceptive threshold which was produced by intraplanter injection of PGE2, and which has been shown to be entirely dependent on capsaicin-sensitive afferents, was not affected by treatment with this NK1 receptor antagonist. These results show that systemic administration of SR140333, at doses which cause inhibition of neurogenic inflammation, has no detectable effect on acute chemo- or thermonociception in conscious rats.
在麻醉大鼠中,神经激肽(NK)1受体拮抗剂SR140333(10 - 1000微克/千克)对芥子油诱导的后爪背部皮肤血浆蛋白外渗具有立体选择性抑制作用。皮下注射SR140333后,血浆蛋白外渗的抑制作用在注射后3小时达到最大。静脉注射0.1毫克/千克或皮下注射1.0毫克/千克的剂量产生持久的抑制作用,在治疗后24小时仍具有显著意义。由于已证明全身给药SR140333可抑制麻醉大鼠的伤害性反应,我们想评估SR140333对清醒大鼠化学性和热性伤害感受的可能影响。SR140333(100微克/千克皮下注射)在擦拭试验中并未降低大鼠对辣椒素刺激作用的行为反应,在足底试验中也未影响热伤害感受阈值。此外,足底注射PGE2所产生的热伤害感受阈值降低(已证明完全依赖于辣椒素敏感传入神经)不受该NK1受体拮抗剂治疗的影响。这些结果表明,全身给药SR140333在引起神经源性炎症抑制的剂量下,对清醒大鼠的急性化学性或热性伤害感受没有可检测到的影响。
