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[促甲状腺激素释放激素对吗啡敏感性遗传诱导机制的调节作用]

[The modulating effect of the thyrotropin-releasing hormone on genetically induced mechanisms of morphine sensitivity].

作者信息

Borisova E V, Sudakov S K

出版信息

Zh Vyssh Nerv Deiat Im I P Pavlova. 1995 Nov-Dec;45(6):1174-81.

PMID:8585307
Abstract

The influence of thyrotropin-releasing hormone (TRH) on morphine-induced analgesic and reinforced responses was studied in two inbred strains of rats, Fischer-344 (F344) and Wistar Albino Glaxo/GSto (WAG). Conditioned place preference, voluntary consumption of morphine solution and analgesic action of morphine in tail immersion test were studied. There were interstrain differences in pain sensitivity, i.e., F344 rats had longer latency of tail immersion and deeper analgesic effect of morphine (5 mg/kg, ip) than WAG rats. TRH (1 mg/kg, ip) produced a stronger analgesic effect in WAG rats, while F344 rats demonstrated only slight increase in pain threshold. Administration of TRH in combination with morphine significantly stronger potentiated the effect of the latter in WAG than in F344 rats. F344 rats preferred morphine in the two-bottle choice test and consumed relatively larger amount of morphine solution in the drinking paradigm than WAG rats. Morphine in the dose of 5 mg/kg (ip) induced place preference in both rat strains. Intraventricular administration of TRH (1 mcg) produced a slight effect of place preference only in F344 rats. Preceded by morphine, such injection reduced the effect of place preference. It is suggested that WAG and F344 rats have different sensitivity of brain structures to TRH. This is probably determined by genetic differences in dissociation of analgesic and reinforcing effects of morphine.

摘要

在两种近交系大鼠,即Fischer-344(F344)和Wistar Albino Glaxo/GSto(WAG)中,研究了促甲状腺激素释放激素(TRH)对吗啡诱导的镇痛和强化反应的影响。研究了条件性位置偏爱、吗啡溶液的自愿消耗量以及吗啡在尾部浸没法中的镇痛作用。在疼痛敏感性方面存在品系间差异,即F344大鼠尾部浸入的潜伏期比WAG大鼠长,且吗啡(5mg/kg,腹腔注射)的镇痛效果更深。TRH(1mg/kg,腹腔注射)在WAG大鼠中产生更强的镇痛作用,而F344大鼠仅表现出疼痛阈值略有增加。与吗啡联合给药时,TRH在WAG大鼠中比在F344大鼠中更显著地增强了后者的作用。在双瓶选择试验中,F344大鼠比WAG大鼠更喜欢吗啡,并且在饮水模式下消耗的吗啡溶液量相对更大。5mg/kg(腹腔注射)剂量的吗啡在两种大鼠品系中均诱导了位置偏爱。脑室内注射TRH(1μg)仅在F344大鼠中产生了轻微的位置偏爱效应。在吗啡之前进行这种注射会降低位置偏爱效应。提示WAG和F344大鼠脑结构对TRH的敏感性不同。这可能由吗啡镇痛和强化作用解离的遗传差异所决定。

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