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一氧化氮合酶抑制剂对大鼠腰段脊髓中角叉菜胶性水肿及相关c-Fos表达的抑制作用

Reduction of carrageenin oedema and the associated c-Fos expression in the rat lumbar spinal cord by nitric oxide synthase inhibitor.

作者信息

Honoré P, Chapman V, Buritova J, Besson J M

机构信息

Physiopharmacologie du Systme Nerveux, INSERM U.161, Paris, France.

出版信息

Br J Pharmacol. 1995 Jan;114(1):77-84. doi: 10.1111/j.1476-5381.1995.tb14908.x.

Abstract
  1. Three hours after intraplantar carrageenin (6 mg/150 microliters of saline) Fos-like immunoreactivity (Fos-LI) was mainly observed in L4 and L5 segments of the dorsal horn. Both superficial (I-II) and deep laminae (V-VI) neurones were labelled. 2. We have studied the effect of systemic administration of a nitric oxide synthase inhibitor, NG-nitro-L-arginine methyl ester (L-NAME) on carrageenin evoked c-Fos expression and thus the contribution of nitric oxide to this expression. 3. Pre-administration of L-NAME (10, 25, 50, 100 mg kg-1, i.v.) dose-dependently reduced the number of superificial and deep laminae Fos-LI neurones, 100 mg kg-1 produced a 63 +/- 2% and 72 +/- 4% reduction of Fos-LI neurones respectively, P < 0.0001 for both superficial and deep neurones. 4. Pre-administered L-NAME dose-relatedly reduced the carrageenin-evoked paw and ankle oedema, with 100 mg kg-1 of L-NAME resulting in a 74 +/- 2% and 103 +/- 2% reduction respectively. 5. Post-administration of L-NAME (10 mg kg-1, i.v.) reduced the number of superficial and deep laminae Fos-LI neurones (65 +/- 7% and 53 +/- 8% reduction respectively, P < 0.01 for both superficial and deep neurones). 6. Post-administered L-NAME reduced both the paw and ankle oedema (52 +/- 8% and 62 +/- 10% reduction respectively, P < 0.0001 for both paw and ankle). 7. Pre-administered D-NAME (100 mg kg-1, i.v.), the inactive isomer of L-NAME, produced a weak reduction of the number of superficial laminae Fos-LI neurones (26 +/- 8% reduction, P<0.05), without influencing the deep Fos-LI neurones (5 +/- 8% enhancement) or the oedema.8. Systemic L-arginine (1200 mg kg-1) did not reverse the reduction of the total number of Fos-LI neurones induced by 100mg kg-1 of L-NAME, or the effect of L-NAME on the paw and ankle oedema.9. Intraplantar L-arginine (30 mg) did not reverse the effect of L-NAME (100 mg kg-1) on the total number of Fos-LI neurones. However, the inhibitory effects of L-NAME on the paw and ankle oedema were partially reversed by intraplantar L-Arginine (34 +/- 9% and 45 +/- 11% reduction of carrageenin oedema respectively) with these effects being significant as compared to the effect of L-NAME alone(P<0.05 for both).10. There is a strong correlation between the reduction of the number of Fos-LI neurones and the oedema by L-NAME, clearly demonstrating a predominant role of peripheral NO in the development of one of the signs of carrageenin inflammation.
摘要
  1. 足底注射角叉菜胶(6毫克/150微升生理盐水)3小时后,在背角的L4和L5节段主要观察到Fos样免疫反应性(Fos-LI)。浅层(I-II层)和深层(V-VI层)神经元均被标记。

  2. 我们研究了全身给予一氧化氮合酶抑制剂NG-硝基-L-精氨酸甲酯(L-NAME)对角叉菜胶诱发的c-Fos表达的影响,从而研究一氧化氮对这种表达的作用。

  3. 预先给予L-NAME(10、25、50、100毫克/千克,静脉注射)剂量依赖性地减少了浅层和深层Fos-LI神经元的数量,100毫克/千克分别使Fos-LI神经元数量减少63±2%和72±4%,浅层和深层神经元的P均<0.0001。

  4. 预先给予L-NAME剂量相关地减少了角叉菜胶诱发的爪部和踝部水肿,100毫克/千克的L-NAME分别导致减少74±2%和103±2%。

  5. 给予L-NAME(10毫克/千克,静脉注射)后,减少了浅层和深层Fos-LI神经元的数量(分别减少65±7%和53±8%,浅层和深层神经元的P均<0.01)。

  6. 给予L-NAME后减少了爪部和踝部水肿(分别减少52±8%和62±10%,爪部和踝部的P均<0.0001)。

  7. 预先给予L-NAME的无活性异构体D-NAME(100毫克/千克,静脉注射)使浅层Fos-LI神经元数量略有减少(减少26±8%,P<0.05),但不影响深层Fos-LI神经元(增加5±8%)或水肿。

  8. 全身给予L-精氨酸(1200毫克/千克)并未逆转100毫克/千克L-NAME诱导的Fos-LI神经元总数的减少,也未逆转L-NAME对爪部和踝部水肿的影响。

  9. 足底注射L-精氨酸(30毫克)并未逆转L-NAME(100毫克/千克)对Fos-LI神经元总数的影响。然而,足底注射L-精氨酸部分逆转了L-NAME对爪部和踝部水肿的抑制作用(角叉菜胶水肿分别减少34±9%和45±11%),与单独使用L-NAME的作用相比,这些作用具有显著性(两者P均<0.05)。

  10. L-NAME减少Fos-LI神经元数量与水肿之间存在很强的相关性,清楚地表明外周一氧化氮在角叉菜胶炎症的一个体征发展中起主要作用。

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