氯胺酮通过NO通路介导的抗伤害作用与抑制脊髓P物质受体研究

张博; 王宏; 张涤非; 张博; 王宏; 张涤非

doi:10.13898/j.cnki.issn.1000-2200.2016.01.003

[1]

TAKAHASHI T,KINOSHITA M,SHONO S,et al. The effect of ketamine anesthesia on the immune function of mice with postoperative septicemia[J]. Anesth Analg,2010,111(4):1051.

[2]

NADESON R,TUCKER A,BAJUNAKI E,et al. Potentiation by ketamine of fentanyl antinociception. I. An experimental study in rats showing that ketamine administere by non-spinal routes targets spinal cord antinociceptive systems[J]. Br J Anaesth, 2002,88(5):685.

[3]

ZHOU ZS,ZHAO ZQ. Ketamine blockage of both tetrodotoxin(TTX)-sensitive and TTX-resistant sodium channels of rat dorsal root ganglion neurons[J]. Brain Res Bull,2000,52(50):427.

[4]

CASTROMAN PJ,NESS TJ. Ketamine,an N-methyl-D-aspartate receptor antagonist, inhibits the spinal neuronal responses to distension of the rat urinary bladder[J]. Anesthesiology,2002,96(6):1410.

[5]

HAO JX,SJOLUND BH,WIESENFELD-HALLIN Z. Electrophysiological evidence for an antinociceptive effect of ketamine in the rat spinal cord[J].Acta Anaesthesiol Scand,1998,42(4):435.

[6]

LAURIDO C,PELISSIER T,PEREZ H,et al. Effect of ketamine on spinal cord nociceptive transmission in normal and monoarthritic rats[J]. Neuroreport,2001,12(8):1551.

[7]

THOMSON LM,TERMAN GW,ZENG J,et al. Decreased substance P and NK1 receptor immumoreactivity and function in the spinal cord dorsal horn of morphine-treated neonatal rats[J]. J Pain,2008,9(1):11.

[8]

TAKAHASI K,SAKURADA T,SAKURADA S,et al. Behavioural characterization of substance P-induced nociceptive response in mice[J]. Neuropharmacology,1987,26(9):1289.

[9]

KISARA K,TAN-NO K,SAKURADA T. Pharmacological profile of sendide,a tachykinin NK-1 receptor antagonist[J]. Nippon Yakurigaku Zasshi,1997,110(6):315.

[10]

OKAMOTO T, MINSMI K, UEZONO Y, et al. The inhibitory effects of ketamine and pentobarbital on substance p receptors expressed in xenopus oocytes[J]. Anesth Analg,2003,97(1):104.

[11]

SONG XJ, ZHAO ZQ. Interaction between substance P and excitatory amino acid receptors in modulation of nociceptive responses of cat spinal dorsal horn neurons[J]. Neurosci Lett, 1994,168(1/2):49.

[12]

TONNER PH,SCHOLZ J,LAMBERZ L,et al. Inhibition of nitric oxide synthase decreases anesthetic requirements of intravenous anesthetics in Xenopus laevis[J]. Anesthesiology,1997,87(6):1479.

[13]

GALLEY HF,WEBSTER NR. Brain nitric oxide synthase activity is decreased by intravenous anesthetics[J]. Anesth Analg,1996, 83(3):591.

[14]

颜明,曾因明,张励才,等. 大鼠脊髓神经元对福尔马林痛刺激的反应及氯胺酮的调节[J]. 解剖学通报,2003,26(3):209.

[15]

袁维秀,张宏,徐娟,等. 鞘内注射氯胺酮对慢性神经痛大鼠脊髓背角一氧化氮合酶的影响[J]. 中华麻醉学杂志,2004, 204(5):377.

[16]

BULUTCU F,DOGRUL A,GÜÇMO. The involvement of nitric oxide in the analgesic effects of ketamine[J]. Life Sci,2002,71(7):841.

[17]

孙晓彩,李文斌,李淑琴,等. 鞘内注射神经激肽-1受体激动剂Sar-SP增强大鼠脊髓一氧化氮合酶表达和一氧化氮生成[J]. 生理学报,2003,55(6):677.