速激肽NK1和NK2受体对大鼠脊髓兴奋性氨基酸反应性的内源性调节

Endogenous modulation of excitatory amino acid responsiveness by tachykinin NK1 and NK2 receptors in the rat spinal cord.

作者信息

Chizh B A, Cumberbatch M J, Birch P J, Headley P M

机构信息

Department of Physiology, University of Bristol, School of Medical Sciences.

出版信息

Br J Pharmacol. 1995 Jul;115(6):1013-9. doi: 10.1111/j.1476-5381.1995.tb15912.x.

DOI:10.1111/j.1476-5381.1995.tb15912.x

PMID:7582497

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1908992/

Abstract

The effects of selective tachykinin (neurokinin, NK) NK1 and NK2 receptor antagonists have been examined on spinal neurones in alpha-chloralose anaesthetized, spinalized rats. They were tested for effects on responses both to excitatory amino acids (EAA) and to noxious heat stimuli. They were also tested for their ability to reverse the actions of selective NK agonists. 2. The NK1-selective antagonists GR82334 (peptide) and CP-99,994 (non-peptide), when applied by microiontophoresis, both reduced responses to kainate > AMPA > NMDA. Intravenous CP-99,994 (3 mg kg-1) also reduced responses to kainate but had inconsistent effects on nociceptive responses. 3. GR82334, applied microiontophoretically, reduced the enhancement by the selective NK1 agonist, GR73632 of both responses to EAAs and background activity. Systemic CP-99,994 (< or = 10 mg kg-1) failed to reverse the effects of GR73632. 4. The selective peptide NK2 antagonist, GR103537, had no consistent effects on responses to EAAs when applied by iontophoresis. In contrast, the non-peptide NK2 antagonist, GR159897, administered systemically (0.5-2 mg kg-1, i.v.) enhanced responses to kainate (but not NMDA); responses to noxious heat were enhanced only weakly. 5. Iontophoretically-administered GR103537 attenuated the effects of the NK2 agonist GR64349, which selectively reduced responses to kainate compared to those to NMDA. Systemically administered GR159897 (< or = 2 mg kg-1, i.v.) caused little antagonism of the effects of GR64349. 6. The data indicate that under these conditions the non-peptide antagonists are not reliable at reversing the actions of selective NK agonists. 7. These results suggest that there is a tonic release of endogenous tachykinins that can modulate glutamatergic neurotransmission in the spinal cord. They provide further support for the hypothesis that release of endogenous NKs acting on NK1 and NK2 receptors can promote NMDA receptor mediated glutamatergic transmission.

摘要

研究了选择性速激肽（神经激肽，NK）NK1和NK2受体拮抗剂对α-氯醛糖麻醉、脊髓横断大鼠脊髓神经元的作用。检测了它们对兴奋性氨基酸（EAA）反应和有害热刺激反应的影响。还检测了它们逆转选择性NK激动剂作用的能力。2. NK1选择性拮抗剂GR82334（肽类）和CP-99,994（非肽类）经微量离子电泳给药时，均降低了对 kainate＞AMPA＞NMDA的反应。静脉注射CP-99,994（3mg/kg）也降低了对kainate的反应，但对伤害性反应的影响不一致。3. 经微量离子电泳给药的GR82334降低了选择性NK1激动剂GR73632对EAA反应和背景活动的增强作用。全身性CP-99,994（≤10mg/kg）未能逆转GR73632的作用。4. 选择性肽类NK2拮抗剂GR103537经离子电泳给药时，对EAA反应无一致影响。相比之下，非肽类NK2拮抗剂GR159897全身性给药（0.5 - 2mg/kg，静脉注射）增强了对kainate的反应（但对NMDA无增强作用）；对有害热的反应仅轻微增强。5. 经离子电泳给药的GR103537减弱了NK2激动剂GR64349的作用，与对NMDA的反应相比，GR64349选择性降低了对kainate的反应。全身性给药的GR159897（≤2mg/kg，静脉注射）对GR64349的作用几乎没有拮抗作用。6. 数据表明，在这些条件下非肽类拮抗剂在逆转选择性NK激动剂的作用方面不可靠。7. 这些结果表明，内源性速激肽存在紧张性释放，可调节脊髓中的谷氨酸能神经传递。它们为内源性NK作用于NK1和NK2受体可促进NMDA受体介导的谷氨酸能传递这一假说提供了进一步支持。