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Effects of general anesthetics on substance p release and c-fos expression in the spinal dorsal horn

机译:全身麻醉药对脊髓背角p物质释放和c-fos表达的影响

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BACKGROUND: The authors examined in vivo the effects of general anesthetics on evoked substance P release (primary afferent excitability) and c-Fos expression (neuronal activation) in superficial dorsal horn. METHODS: Rats received saline, propofol (100 mg/kg), pentobarbital (50 mg/kg), isoflurane (2 minimum alveolar concentration), nitrous oxide (66%), or fentanyl (30 μg/kg). During anesthesia, rats received intraplantar 5% formalin (50 μl) to left hind paw. Ten minutes later, rats underwent transcardial perfusion with 4% paraformaldehyde. Substance P release from small primary afferents was assessed by incidence of neurokinin 1 receptor internalization in the superficial dorsal horn. In separate studies, rats were sacrificed after 2 h and c-Fos expression measured. RESULTS: Intraplantar formalin-induced robust neurokinin 1 receptor internalization in ipsilateral dorsal horn (ipsilateral: 54 ± 6% [mean ± SEM], contralateral: 12 ± 2%; P < 0.05; n = 4). Fentanyl, but not propofol, pentobarbital, isoflurane, nor nitrous oxide alone inhibited neurokinin 1 receptor internalization. However, 2 minimum alveolar concentration isoflurane + nitrous oxide reduced neurokinin 1 receptor internalization (27 ± 3%; P < 0.05; n = 5). All agents reduced c-Fos expression (control: 34 ± 4, fentanyl: 8 ± 2, isoflurane: 12 ± 3, nitrous oxide: 11 ± 2, isoflurane + nitrous oxide: 12 ± 1, pentobarbital: 11 ± 2, propofol: 13 ± 3; P < 0.05; n = 3). CONCLUSION: General anesthetics at anesthetic concentrations block spinal neuron activation through a mechanism that is independent of an effect on small primary afferent peptide release. The effect of fentanyl alone and the synergistic effect of isoflurane and nitrous oxide on substance P release suggest a correlative rationale for the therapeutic use of these anesthetic protocols by blocking nociceptive afferent transmitter release and preventing the initiation of cascade, which is immediately postsynaptic to the primary afferent.
机译:背景:作者在体内检查了全身麻醉药对浅表背角诱发的P物质释放(主要传入兴奋性)和c-Fos表达(神经元激活)的影响。方法:大鼠接受生理盐水,异丙酚(100 mg / kg),戊巴比妥(50 mg / kg),异氟烷(2最低肺泡浓度),一氧化二氮(66%)或芬太尼(30μg/ kg)。麻醉期间,大鼠左脚后掌接受5%的福尔马林(50μl)。十分钟后,大鼠接受4%多聚甲醛经心灌注。通过浅表背角内神经激肽1受体内在的发生率评估了小原发灶中P物质的释放。在单独的研究中,在2 h后处死大鼠并测量c-Fos表达。结果:同侧背角plant内福尔马林诱导的稳健神经激肽1受体内在化(同侧:54±6%[平均值±SEM],对侧:12±2%; P <0.05; n = 4)。芬太尼,但不是丙泊酚,戊巴比妥,异氟烷,也不是一氧化二氮单独抑制神经激肽1受体的内在化。然而,2个最低肺泡浓度异氟烷+一氧化二氮降低了神经激肽1受体的内在化(27±3%; P <0.05; n = 5)。所有药物均降低c-Fos表达(对照:34±4,芬太尼:8±2,异氟烷:12±3,一氧化二氮:11±2,异氟烷+一氧化二氮:12±1,戊巴比妥:11±2,异丙酚: 13±3; P <0.05; n = 3)。结论:麻醉药在麻醉浓度下会通过独立于对小的初级传入肽释放的影响的机制来阻断脊髓神经元的活化。单独芬太尼的作用以及异氟烷和一氧化二氮对P物质释放的协同作用通过阻断伤害性传入递质的释放并阻止级联反应的发生,提示了这些麻醉方案在治疗上的使用,这是一个相关的基本原理,该级联反应会在初级突触后立即发生传入。

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