缓激肽和前列腺素对大鼠脊髓体外释放降钙素基因相关肽样免疫反应性的影响。
Effect of bradykinin and prostaglandins on the release of calcitonin gene-related peptide-like immunoreactivity from the rat spinal cord in vitro.
作者信息
Andreeva L, Rang H P
机构信息
Sandoz Institute for Medical Research, London.
出版信息
Br J Pharmacol. 1993 Jan;108(1):185-90. doi: 10.1111/j.1476-5381.1993.tb13460.x.
Abstract
- The release of calcitonin gene-related peptide-like immunoreactivity (CGRP-LI) from the dorsal horn of the rat spinal cord in vitro in response to dorsal root stimulation was measured by radioimmunoassay. 2. Stimulation of the dorsal roots (3 or 4 roots on each side) at 10 Hz for 5 min evoked a mean release (R1) of 134.3 +/- 17.5 (n = 10) fmol CGRP-LI; the release (R2) evoked by a second stimulation period 30 min later under control conditions was 77 +/- 10% (n = 10) of R1. Test compounds were applied to the preparation following release R1, and their effect calculated from the value of R2/R1. 3. Bradykinin (0.01-10 microM) had no significant effect on the basal release of CGRP-LI, but at 0.1-10 microM it increased 2-3 fold the release evoked by dorsal root stimulation. 4. This effect of bradykinin was prevented by indomethacin (10 microM), or by the B2-receptor antagonist, Hoe140 (1-10 microM). In the presence of Hoe140, bradykinin significantly reduced R2/R1; the explanation for this is not clear. 5. The B1-receptor agonist, Des-Arg9-bradykinin (10 microM), did not affect CGRP-LI release nor was the effect of bradykinin blocked by the B1-receptor antagonist, Des-Arg9-Leu8-bradykinin (10 microM). 6. Various prostaglandins were found to mimic the effect of bradykinin on CGRP-LI release. Their approximate order of potency was prostaglandin D2 (PGD2) = PGE1 > PGF2 alpha = PGE2; PGI2 was ineffective at 10 microM.7. Forskolin (30 muM) and 3-isobutyl l-methylxanthine (IBMX; 10 fM) also increased the evoked release of CGRP-LI.8. It is concluded that bradykinin acts on B2-receptors in the spinal cord, causing the formation ofprostanoids, which in turn cause an enhancement of neuropeptide release from primary afferent nerve terminals in the dorsal horn. This effect may be secondary to activation of adenylate cyclase. Because B2-receptors are mainly associated with primary afferent nerve terminals, it is likely that prostanoid production is also a function of these structures. Whether this action of bradykinin has any physiological function in nociceptive transmission remains unclear..
摘要
- 采用放射免疫分析法测定了体外培养的大鼠脊髓背角中降钙素基因相关肽样免疫反应性物质(CGRP-LI)在背根刺激下的释放情况。2. 以10Hz频率刺激背根(每侧3或4根)5分钟,诱发的CGRP-LI平均释放量(R1)为134.3±17.5(n = 10)fmol;30分钟后在对照条件下进行的第二次刺激诱发的释放量(R2)为R1的77±10%(n = 10)。在释放R1后将测试化合物应用于标本,并根据R2/R1的值计算其效果。3. 缓激肽(0.01 - 10μM)对CGRP-LI的基础释放无显著影响,但在0.1 - 10μM时,它使背根刺激诱发的释放量增加2 - 3倍。4. 吲哚美辛(10μM)或B2受体拮抗剂Hoe140(1 - 10μM)可阻止缓激肽的这种作用。在存在Hoe140的情况下,缓激肽显著降低了R2/R1;对此的解释尚不清楚。5. B1受体激动剂去精氨酸9-缓激肽(10μM)不影响CGRP-LI的释放,缓激肽的作用也未被B1受体拮抗剂去精氨酸9-亮氨酸8-缓激肽(10μM)阻断。
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