McGaraughty Steve, Chu Katharine L, Bitner Robert S, Martino Brenda, El Kouhen Rachid, Han Ping, Nikkel Arthur L, Burgard Edward C, Faltynek Connie R, Jarvis Michael F
Neuroscience Research, Global Pharmaceutical Research and Development, Abbott Laboratories, Abbott Park, Illinois 60064, USA.
J Neurophysiol. 2003 Oct;90(4):2702-10. doi: 10.1152/jn.00433.2003. Epub 2003 Jun 18.
It is well established that the vanilloid receptor, VR1, is an important peripheral mediator of nociception. VR1 receptors are also located in several brain regions, yet it is uncertain whether these supraspinal VR1 receptors have any influence on the nociceptive system. To investigate a possible nociceptive role for supraspinal VR1 receptors, capsaicin (10 nmol in 0.4 microl) was microinjected into either the dorsal (dPAG) or ventral (vPAG) regions of the periaqueductal gray. Capsaicin-related effects on tail flick latency (immersion in 52 degrees C water) and on neuronal activity (on-, off-, and neutral cells) in the rostral ventromedial medulla (RVM) were measured in lightly anesthetized rats. Administration of capsaicin into the dPAG but not the vPAG caused an initial hyperalgesic response followed later by analgesia (125 +/- 20.96 min postinjection). The tail flick-related burst in on-cell activity was triggered earlier in the hyperalgesic phase and was delayed or absent during the analgesic phase. Spontaneous activity of on-cells increased at the onset of the hyperalgesic phase and decreased before and during the analgesic phase. The tail flick-related pause in off-cell activity as well as spontaneous firing for these cells was unchanged in the hyperalgesic phase. During the analgesic phase, off-cells no longer paused during noxious stimulation and had increased levels of spontaneous activity. Neutral cell firing was unaffected in either phase. Pretreatment with the VR1 receptor antagonist, capsazepine (10 nmol in 0.4 microl), into the dPAG blocked the capsaicin-induced hyperalgesia as well as the corresponding changes in on- and off-cell activity. VR1 receptor immunostaining was observed in the dPAG of untreated rats. Microinjection of capsaicin likely sensitized and then desensitized dPAG neurons affecting nocifensive reflexes and RVM neuronal activity. These results suggest that supraspinal VR1 receptors in the dPAG contribute to descending modulation of nociception.
众所周知,香草酸受体VR1是伤害感受的重要外周介质。VR1受体也位于多个脑区,但尚不确定这些脊髓上的VR1受体是否对伤害感受系统有任何影响。为了研究脊髓上VR1受体可能的伤害感受作用,将辣椒素(10纳摩尔溶于0.4微升)微量注射到中脑导水管周围灰质的背侧(dPAG)或腹侧(vPAG)区域。在轻度麻醉的大鼠中测量了辣椒素对甩尾潜伏期(浸入52摄氏度水中)以及延髓头端腹内侧(RVM)中神经元活动(开细胞、关细胞和中性细胞)的相关影响。向dPAG而非vPAG注射辣椒素会引起最初的痛觉过敏反应,随后出现镇痛作用(注射后125±20.96分钟)。在痛觉过敏阶段,与甩尾相关的开细胞活动爆发提前触发,而在镇痛阶段则延迟或消失。开细胞的自发活动在痛觉过敏阶段开始时增加,在镇痛阶段之前和期间减少。在痛觉过敏阶段,与甩尾相关的关细胞活动暂停以及这些细胞的自发放电没有变化。在镇痛阶段,关细胞在有害刺激期间不再暂停,且自发放电水平增加。中性细胞放电在两个阶段均未受影响。预先向dPAG注射VR1受体拮抗剂辣椒平(10纳摩尔溶于0.4微升)可阻断辣椒素诱导的痛觉过敏以及开细胞和关细胞活动的相应变化。在未处理大鼠的dPAG中观察到VR1受体免疫染色。微量注射辣椒素可能使dPAG神经元致敏,然后使其脱敏,从而影响伤害性防御反射和RVM神经元活动。这些结果表明,dPAG中的脊髓上VR1受体有助于伤害感受的下行调制。
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