Tonic modulation of spinal hyperexcitability by the endocannabinoid receptor system in a rat model of osteoarthritis pain.

Sagar DR; Staniaszek LE; Okine BN; Woodhams S; Norris LM; Pearson RG; Garle MJ; Alexander SP; Bennett AJ; Barrett DA; Kendall DA; Scammell BE; Chapman V

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Tonic modulation of spinal hyperexcitability by the endocannabinoid receptor system in a rat model of osteoarthritis pain.

机译：内源性大麻素受体系统在骨关节炎疼痛的大鼠模型中对脊髓兴奋性的强直调节。

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OBJECTIVE: To investigate the impact of an experimental model of osteoarthritis (OA) on spinal nociceptive processing and the role of the inhibitory endocannabinoid system in regulating sensory processing at the spinal level. METHODS: Experimental OA was induced in rats by intraarticular injection of sodium mono-iodoacetate (MIA), and the development of pain behavior was assessed. Extracellular single-unit recordings of wide dynamic range (WDR) neurons in the dorsal horn were obtained in MIA-treated rats and saline-treated rats. The levels of endocannabinoids and the protein and messenger RNA levels of the main synthetic enzymes for the endocannabinoids (N-acyl phosphatidylethanolamine phospholipase D [NAPE-PLD] and diacylglycerol lipase alpha [DAGLalpha]) in the spinal cord were measured. RESULTS: Low-weight (10 gm) mechanically evoked responses of WDR neurons were significantly (P < 0.05) facilitated 28 days after MIA injection compared with the responses in saline-treated rats, and spinal cord levels of anandamide and 2-arachidonoyl glycerol (2-AG) were increased in MIA-treated rats. Protein levels of NAPE-PLD and DAGLalpha, which synthesize anandamide and 2-AG, respectively, were elevated in the spinal cords of MIA-treated rats. The functional role of endocannabinoids in the spinal cords of MIA-treated rats was increased via activation of cannabinoid 1 (CB(1) ) and CB(2) receptors, and blockade of the catabolism of anandamide had significantly greater inhibitory effects in MIA-treated rats compared with control rats. CONCLUSION: Our findings provide new evidence for altered spinal nociceptive processing indicative of central sensitization and for adaptive changes in the spinal cord endocannabinoid system in an experimental model of OA. The novel control of spinal cord neuronal responses by spinal cord CB(2) receptors suggests that this receptor system may be an important target for the modulation of pain in OA.

机译：目的：研究骨关节炎（OA）实验模型对脊髓伤害感受性加工的影响，以及抑制性内源性大麻素系统在调节脊髓水平的感觉加工中的作用。方法：通过关节内注射单碘乙酸钠（MIA）诱导大鼠实验性OA，并评估其疼痛行为的发展。在MIA治疗的大鼠和生理盐水治疗的大鼠中，获得了背角中宽动态范围（WDR）神经元的细胞外单单位记录。测量了脊髓中内源性大麻素的水平以及内源性大麻素的主要合成酶（N-酰基磷脂酰乙醇胺磷脂酶D [NAPE-PLD]和二酰基甘油脂酶α[DAGLα]）的蛋白质和信使RNA的水平。结果：MIA注射后28天，轻量（10 gm）引起的WDR神经元机械诱发反应显着（P <0.05）促进，与盐水处理的大鼠，脊髓中花生四烯酸酰胺和2-花生四烯酸甘油酯（在经MIA处理的大鼠中2-AG）升高。在MIA处理的大鼠的脊髓中，分别合成anandamide和2-AG的NAPE-PLD和DAGLalpha的蛋白质水平升高。通过激活大麻素1（CB（1））和CB（2）受体，内源性大麻素在MIA处理的大鼠的脊髓中的功能增强，而对MMC处理的Anandamide分解代谢的抑制作用则明显更大大鼠与对照大鼠相比。结论：我们的发现为OA实验模型中指示中央敏化的改变的脊髓伤害感受处理以及脊髓内源性大麻素系统的适应性变化提供了新的证据。脊髓CB（2）受体对脊髓神经元反应的新型控制表明，该受体系统可能是OA疼痛调节的重要靶标。

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《Arthritis and Rheumatism》 |2010年第12期|共11页
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Sagar DR; Staniaszek LE; Okine BN; Woodhams S; Norris LM; Pearson RG; Garle MJ; Alexander SP; Bennett AJ; Barrett DA; Kendall DA; Scammell BE; Chapman V;
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中图分类免疫性疾病;
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1. Tonic modulation of spinal hyperexcitability by the endocannabinoid receptor system in a rat model of osteoarthritis pain. [J] . Sagar DR, Staniaszek LE, Okine BN, Arthritis and Rheumatism . 2010,第12期

机译：内源性大麻素受体系统在骨关节炎疼痛的大鼠模型中对脊髓兴奋性的强直调节。
2. Tonic modulation of spinal hyperexcitability by the endocannabinoid receptor system in a rat model of osteoarthritis pain. [J] . Sagar DR, Staniaszek LE, Okine BN, Arthritis and Rheumatism . 2010,第12期

机译：内源性大麻素受体系统在骨关节炎疼痛的大鼠模型中对脊髓兴奋性的强直调节。
3. Tonic modulation of spinal hyperexcitability by the endocannabinoid receptor system in a rat model of osteoarthritis pain † [J] . Devi Rani Sagar, Lydia E. Staniaszek, Bright N. Okine, Arthritis & Rheumatism . 2010,第12期

机译：内源性大麻素受体系统在骨关节炎疼痛大鼠模型中对脊髓兴奋性的强直调节作用†
4. Tonic Effects of BAM8-22, an Agonist at the Novel Sensory Neuron Specific Receptor, on the Nociceptive Flexor Reflex in Rats [C] . Chang Qing Cao, Andy Dray, Martin N. Perkins World Congress on Pain . 2003

机译：作者：张莹莹，王莹，王莹，王莹，王莹，王莹，王莹，王莹，王莹，王莹，王莹,非
5. Development of spinal neuronal hyperexcitability and structural plasticity after cervical facet injury: Implications for modulating persistent pain. [D] . Crosby, Nathan D. 2014

机译：颈椎小面损伤后脊髓神经元过度兴奋和结构可塑性的发展：对持续性疼痛的调节作用。
6. Tonic Modulation of Spinal Hyperexcitability by the Endocannabinoid Receptor System in a Rat Model of Osteoarthritis Pain [O] . Devi Rani Sagar, Lydia E Staniaszek, Bright N Okine, -1

机译：内源性大麻素受体系统在骨关节炎性疼痛大鼠模型中对脊髓兴奋性的强直调节
7. Tonic Modulation of Spinal Hyperexcitability by the Endocannabinoid Receptor System in a Rat Model of Osteoarthritis Pain [O] . Sagar, Devi Rani, Staniaszek, Lydia E, Okine, Bright N, 2010

机译：内源性大麻素受体系统在骨关节炎性疼痛大鼠模型中对脊髓兴奋性的强直调节

Tonic modulation of spinal hyperexcitability by the endocannabinoid receptor system in a rat model of osteoarthritis pain.

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