中脑导水管周围灰质疼痛调节系统中代谢型谷氨酸受体与NMDA谷氨酸受体之间的相互作用。
Interaction between metabotropic and NMDA glutamate receptors in the periaqueductal grey pain modulatory system.
作者信息
Berrino L, Oliva P, Rossi F, Palazzo E, Nobili B, Maione S
机构信息
Department of Experimental Medicine, Section of Pharmacology L. Donatelli, Faculty of Medicine and Surgery, Second University of Naples, Via Costantinopoli 16, 80138 Naples, Italy.
出版信息
Naunyn Schmiedebergs Arch Pharmacol. 2001 Nov;364(5):437-43. doi: 10.1007/s002100100477.
The formalin test was used to investigate the interactive role of periaqueductal grey (PAG) N-methyl-D-aspartate (NMDA) and metabotropic glutamate (mGlu) receptors in the modulation of persistent noxious stimulation in mice. Intra-PAG microinjections of 1 or 3 nmol NMDA, a selective agonist at NMDA-subtype receptors, decreased the nociceptive response (-94+/-5% with 3 nmol) during the latter phase of the test. This effect was antagonized by MK-801, a selective antagonist at NMDA receptors. No change in the early nociceptive phase was observed after NMDA injection. Pretreatment either with 2-methyl-6-phenylethynylpyridine (MPEP, 25 nmol/mouse), a selective antagonist at mGlu5 receptors, or with (2S)-alpha-ethylglutamic acid [(2S)-alpha-EGlu, 30 nmol/mouse], a selective antagonist at group-II mGluRs, prevented the NMDA-induced antinociceptive effect during the late hyperalgesic phase. Pretreatment with (R,S)-alpha-methylserine-O-phosphate [(R,S)-alpha-MSOP, 70 nmol/mouse], a selective antagonist at group-III mGlu receptors, had no effect on the NMDA-induced antinociception. None of the antagonists changed the formalin-induced nociceptive behaviour per se with the dosages used in combination with NMDA. MPEP at 50 nmol/mouse, however, potentiated the early nociceptive phase whilst 100 nmol/mouse attenuated the late phase. Similarly, at the higher dose of 140 nmol/mouse, (R,S)-alpha-MSOP decreased the late hyperalgesic phase. These results provide additional evidence that NMDA and mGlu receptors participate in modulating the hyperalgesia induced by peripheral noxious stimulation. In particular, mGlu receptors may modulate the NMDA receptors in the PAG since their physiological stimulation seems to be required for the NMDA-induced effect. This suggests that, together with ionotropic glutamate receptors, mGlu receptors also play a role in modulating a type of spinal cord neuroplasticity (i.e. wind-up) that has been proposed to mediate hyperalgesia.
采用福尔马林试验研究中脑导水管周围灰质(PAG)N-甲基-D-天冬氨酸(NMDA)和代谢型谷氨酸(mGlu)受体在调节小鼠持续性伤害性刺激中的相互作用。向PAG内微量注射1或3 nmol NMDA(一种NMDA亚型受体的选择性激动剂),可在试验后期降低伤害性反应(3 nmol时为-94±5%)。该效应被NMDA受体的选择性拮抗剂MK-801所拮抗。注射NMDA后,早期伤害性阶段未观察到变化。用mGlu5受体的选择性拮抗剂2-甲基-6-苯基乙炔基吡啶(MPEP,25 nmol/只小鼠)或II组mGluRs的选择性拮抗剂(2S)-α-乙基谷氨酸[(2S)-α-EGlu,30 nmol/只小鼠]预处理,可在痛觉过敏后期阻止NMDA诱导的抗伤害感受作用。用III组mGlu受体的选择性拮抗剂(R,S)-α-甲基丝氨酸-O-磷酸[(R,S)-α-MSOP,70 nmol/只小鼠]预处理,对NMDA诱导的抗伤害感受作用无影响。在与NMDA联合使用的剂量下,这些拮抗剂本身均未改变福尔马林诱导的伤害性行为。然而,50 nmol/只小鼠的MPEP增强了早期伤害性阶段,而100 nmol/只小鼠的MPEP减弱了后期阶段。同样,在140 nmol/只小鼠的较高剂量下,(R,S)-α-MSOP降低了后期痛觉过敏阶段。这些结果提供了额外的证据,表明NMDA和mGlu受体参与调节外周伤害性刺激诱导的痛觉过敏。特别是,mGlu受体可能调节PAG中的NMDA受体,因为它们的生理刺激似乎是NMDA诱导效应所必需的。这表明,与离子型谷氨酸受体一起,mGlu受体在调节一种被认为介导痛觉过敏的脊髓神经可塑性(即wind-up)中也发挥作用。
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