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首页> 外文期刊>American Journal of Physiology >NK(1) receptor and its interaction with NMDA receptor in spinal c-fos expression after lower urinary tract irritation.
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NK(1) receptor and its interaction with NMDA receptor in spinal c-fos expression after lower urinary tract irritation.

机译:下尿路刺激后脊髓c-fos表达中的NK(1)受体及其与NMDA受体的相互作用。

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The role of neurokinin 1 (NK(1)) receptor and possible interaction between NK(1) and N-methyl-D-aspartic acid (NMDA) glutamatergic receptors were investigated on spinal c-fos expression after lower urinary tract irritation with acetic acid infusion in rats. At both levels of the first (L(1)) and sixth lumbar (L(6)) spinal cord, where most of hypogastric nerve and pelvic nerve afferent terminals project, respectively, the selective NK(1) receptor antagonist CP-99,994 dose dependently reduced the total number of c-fos protein (Fos)-positive cells. However, CP-100,263, the enantiomer of CP-99,994 with a very low affinity for NK(1) receptor, did not have any effect on the total number of Fos-positive cells. Coadministration of a low dose (1 mg/kg) of CP-99,994 and NMDA receptor antagonist (MK-801), either of which alone did not affect c-fos expression, significantly inhibited c-fos expression at both levels of the spinal cord. Regarding regional differences, the number of Fos-positive cells decreased significantly at all regions of the L(6) level, but only at the dorsal horn of the L(1) level. These results indicate that NK(1) receptor is involved in spinal c-fos expression after lower urinary tract irritation and that NK(1) and NMDA receptors have a synergistic interaction in the spinal processing of nociceptive input from the lower urinary tract.
机译:研究了神经激肽1(NK(1))受体的作用以及NK(1)与N-甲基-D-天冬氨酸(NMDA)谷氨酸能受体之间可能的相互作用,研究了乙酸对下尿路的刺激后脊髓c-fos表达的变化。输注大鼠。在第一(L(1))和第六腰(L(6))脊髓的两个水平上,分别向腹下神经和骨盆神经的大部分传入末端伸出,选择性NK(1)受体拮抗剂CP-99,994剂量依赖地减少了c-fos蛋白(Fos)阳性细胞的总数。但是,CP-100,263,CP-99,994的对映体,对NK(1)受体的亲和力很低,对Fos阳性细胞总数没有任何影响。低剂量(1 mg / kg)的CP-99,994和NMDA受体拮抗剂(MK-801)的共同给药(均不影响c-fos表达)在两个脊髓水平上均显着抑制c-fos表达。关于区域差异,Fos阳性细胞的数量在L(6)水平的所有区域均显着下降,但仅在L(1)水平的背角处下降。这些结果表明,NK(1)受体参与下尿路刺激后的脊髓c-fos表达,并且NK(1)和NMDA受体在来自下尿路的伤害性输入的脊髓处理中具有协同相互作用。

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