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Endogenous morphine modulates acute thermonociception in mice.

机译:内源性吗啡调节小鼠的急性热伤害感受。

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摘要

The endogenous synthesis of morphine has been clearly demonstrated throughout the phylogenesis of the nervous system of mammals and lower animals. Endogenous morphine, serving as either a neurotransmitter or neurohormone, has been demonstrated in the nervous system of both vertebrates and invertebrates. As one of the effects of exogenous morphine is the modulation of pain perception, we investigated the effects that the depletion of endogenous morphine had on nociceptive transmission. The immunoneutralization of endogenous morphine from brain extracellular spaces was obtained through the intracerebroventricular administration of affinity purified anti-morphine IgG to mice, which then underwent the hot plate test. Endogenous morphine immunoneutralization decreased thermal response latency and attenuated the anti-nociceptive effect of the mu selective agonist DAMGO in hot plate test suggesting that endogenous morphine is involved in pain modulation.
机译:在哺乳动物和低等动物的神经系统的整个系统发育过程中,已清楚地证明了吗啡的内源性合成。在脊椎动物和无脊椎动物的神经系统中均已证明内源性吗啡既可作为神经递质,又可作为神经激素。由于外源性吗啡的作用之一是调节疼痛感,因此我们研究了内源性吗啡消耗对伤害性传递的影响。脑室内通过向小鼠脑室内施用亲和纯化的抗吗啡IgG获得内源性吗啡的免疫中和作用,然后进行热板测试。内源性吗啡免疫中和减少了热选择试验中mu选择性激动剂DAMGO的热反应潜伏期,并减弱了其伤害感受力,表明内源性吗啡参与了疼痛调节。

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