Possible involvement of L-arginine-nitric oxide pathway in the modulation of stress-induced analgesia.

I Hăulică, A Busuioc, C Neamţu, V Dorneanu, G Titu, A Spac
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Abstract

The possible participation of NO in the pain modulation and stress analgesia was studied in Wistar adult rats. Cerebral citruline as a stoichiometric coproduct of NO from L-arginine increased from the mean value 5.6 +/- 0.4 nM/mg.Pt. to 8.9 +/- 0.5 nM/mg.Pt. in acute immobilization stress. Intraperitoneal administration of L-arginine caused only in high doses (50 mg/kg body weight) a small transient decrease of tail-flick latencies to the thermoalgesic stimulus, without significant changes of the stress analgesia induced by the restraint stress. In the pretreated animals with L-NAME a progressive increase of latency time was obtained and the increased latencies induced by acute immobilization appeared significantly potentiated. These results offer new indirect evidence in favour of the modulatory role of NO in the thermoalgesic sensitivity and stress induced analgesia.

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l -精氨酸-一氧化氮通路可能参与应激性镇痛的调节。
研究一氧化氮在Wistar成年大鼠疼痛调节和应激镇痛中的作用。脑瓜氨酸作为l -精氨酸NO的化学计量副产物从平均值5.6 +/- 0.4 nM/mg.Pt增加。8.9±0.5 nM/mg.Pt。在急性固定应力。腹腔注射l-精氨酸仅在高剂量(50 mg/kg体重)下引起对热痛刺激的甩尾潜伏期短暂性小幅度下降,而抑制应激引起的应激镇痛无明显变化。经L-NAME预处理的小鼠潜伏期逐渐增加,急性固定引起的潜伏期明显增强。这些结果为NO在热痛敏感性和应激性镇痛中的调节作用提供了新的间接证据。
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