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[人降钙素对伤害性刺激反应及吗啡镇痛作用的影响]

[Effects of human calcitonin on the response to noxious stimuli and morphine-antinociception].

作者信息

Yamamoto H, Ozaki M, Kishioka S, Iguchi Y, Tamura S

出版信息

Nihon Yakurigaku Zasshi. 1985 Jan;85(1):33-48. doi: 10.1254/fpj.85.33.

Abstract

Effects of human calcitonin (HCT) on the responses of mice and rats to noxious stimuli of various types and morphine-antinociception in the mice tail-pinch method were studied as compared with procine calcitonin (PCT). I.c.v. administration of HCT (0.007-0.071 mg/mouse) delayed response time to tail-pinch stimuli and suppressed acetic acid writhing dose-relatedly. PCT (0.5-3 U/mouse, i.c.v.) exerted a dose-related antinociceptive effect in the tail-pinch and acetic acid writhing methods. The antinociceptive effect was also produced by s.c. administration of HCT (0.071-7.1 mg/kg) and PCT (10-1000 U/kg) in the tail-pinch and writhing methods, while the antinociceptive effect was not detected by the tail-flick method following i.c.v. and s.c. administration of HCT and PCT. Increase in response threshold in the hind paw pressure test was produced by 0.071-7.1 mg/kg, s.c. of HCT and 10-1000 U/kg, s.c. of PCT in rats. Inhibition of writhing due to i.c.v. administration of HCT and PCT was not antagonized by naloxone. Pre-drug control response time to tail-pinch stimuli tended to be shortened after 7-14 days of s.c. treatment with CT, especially with PCT. Pretreatment with HCT and PCT exerted no obvious influence on their acute effects. Morphine-antinociception in the tail-pinch method tended to be potentiated by single s.c. dose of HCT and to be decreased by 14 days chronic s.c. treatment with HCT. The role of calcium in HCT action was discussed.

摘要

将人降钙素(HCT)与猪降钙素(PCT)进行比较,研究了其对小鼠和大鼠多种类型伤害性刺激反应以及小鼠夹尾法中吗啡镇痛作用的影响。脑室内注射HCT(0.007 - 0.071毫克/小鼠)可延迟对夹尾刺激的反应时间,并剂量依赖性地抑制醋酸扭体反应。PCT(0.5 - 3单位/小鼠,脑室内注射)在夹尾法和醋酸扭体法中发挥剂量依赖性镇痛作用。皮下注射HCT(0.071 - 7.1毫克/千克)和PCT(10 - 1000单位/千克)在夹尾法和扭体法中也产生镇痛作用,而脑室内和皮下注射HCT及PCT后,甩尾法未检测到镇痛作用。皮下注射0.071 - 7.1毫克/千克的HCT和10 - 1000单位/千克的PCT可使大鼠后爪压力试验中的反应阈值升高。脑室内注射HCT和PCT引起的扭体抑制未被纳洛酮拮抗。皮下注射CT,尤其是PCT 7 - 14天后,夹尾刺激的给药前对照反应时间往往缩短。HCT和PCT预处理对其急性作用无明显影响。夹尾法中,单次皮下注射HCT倾向于增强吗啡镇痛作用,而皮下注射HCT慢性处理14天则使其降低。讨论了钙在HCT作用中的作用。

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