首页> 外文期刊>American Journal of Physiology >Activation of slowly conducting medullary raphe-spinal neurons, including serotonergic neurons, increases cutaneous sympathetic vasomotor discharge in rabbit.
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Activation of slowly conducting medullary raphe-spinal neurons, including serotonergic neurons, increases cutaneous sympathetic vasomotor discharge in rabbit.

机译:包括血清素能神经元在内的缓慢传导的髓鞘-脊髓神经元的激活会增加兔皮肤的交感性血管舒缩放电。

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摘要

Neurons in the rostral medullary raphe/parapyramidal region regulate cutaneous sympathetic nerve discharge. Using focal electrical stimulation at different dorsoventral raphe/parapyramidal sites in anesthetized rabbits, we have now demonstrated that increases in ear pinna cutaneous sympathetic nerve discharge can be elicited only from sites within 1 mm of the ventral surface of the medulla. By comparing the latency to sympathetic discharge following stimulation at the ventral raphe site with the corresponding latency following stimulation of the spinal cord [third thoracic (T3) dorsolateral funiculus] we determined that the axonal conduction velocity of raphe-spinal neurons exciting ear pinna sympathetic vasomotor nerves is 0.8 +/- 0.1 m/s (n = 6, range 0.6-1.1 m/s). Applications of the 5-hydroxytryptamine (HT)(2A) antagonist trans-4-((3Z)3-[(2-dimethylaminoethyl)oxyimino]-3-(2-fluorophenyl)propen-1 -yl)-phenol, hemifumarate (SR-46349B, 80 microg/kg in 0.8 ml) to the cerebrospinal fluid above thoracic spinal cord (T1-T7), but not the lumbar spinal cord (L2-L4), reduced raphe-evoked increases in ear pinna sympathetic vasomotor discharge from 43 +/- 9 to 16 +/- 6% (P < 0.01, n = 8). Subsequent application of the excitatory amino acid (EAA) antagonist kynurenic acid (25 micromol in 0.5 ml) substantially reduced the remaining evoked discharge (22 +/- 8 to 6 +/- 6%, P < 0.05, n = 5). Our conduction velocity data demonstrate that only slowly conducting raphe-spinal axons, in the unmyelinated range, contribute to sympathetic cutaneous vasomotor discharge evoked by electrical stimulation of the medullary raphe/parapyramidal region. Our pharmacological data provide evidence that raphe-spinal neurons using 5-HT as a neurotransmitter contribute to excitation of sympathetic preganglionic neurons regulating cutaneous vasomotor discharge. Raphe-spinal neurons using an EAA, perhaps glutamate, make a substantial contribution to the ear sympathetic nerve discharge evoked by raphe stimulation.
机译:延髓延髓缝/锥体旁区域的神经元调节皮肤交感神经放电。现在,在麻醉的兔子的不同腹背沟/旁锥体部位使用聚焦电刺激,我们已经证明,仅可从延髓腹面1 mm内的部位引起耳廓皮肤交感神经放电的增加。通过比较腹股沟部位刺激后交感神经放电的潜伏期与脊髓[第三胸(T3)背外侧功能的刺激后相应潜伏期”的比较,我们确定了刺激耳廓交感性血管舒缩的椎间隙神经元的轴突传导速度。神经为0.8 +/- 0.1 m / s(n = 6,范围为0.6-1.1 m / s)。 5-羟基色胺(HT)(2A)拮抗剂反式-4-((3Z)3-[(2-二甲基氨基乙基)氧亚氨基] -3-(2-氟苯基)丙烯-1-基)苯酚,半富马酸酯的应用( SR-46349B,在80 ml / kg(0.8毫升中)至胸脊髓(T1-T7)上方的脑脊液,而不是腰脊髓(L2-L4),降低了由耳蜗引起的耳突交感性血管舒缩放电43 +/- 9至16 +/- 6%(P <0.01,n = 8)。随后施加兴奋性氨基酸(EAA)拮抗剂强尿酸(0.5毫升中的25微摩尔)可以显着降低剩余的诱发放电(22 +/- 8至6 +/- 6%,P <0.05,n = 5)。我们的传导速度数据表明,只有在非髓鞘范围内缓慢传导的沟脊脊髓轴突,才可通过电刺激髓质沟/旁锥体区域诱发交感性皮肤血管舒缩。我们的药理数据提供了证据,表明使用5-HT作为神经递质的缝质-脊髓神经元可促进交感神经节前神经元的兴奋,从而调节皮肤血管舒缩放电。使用EAA(可能是谷氨酸)的鼻沟神经元对由鼻沟刺激引起的耳交感神经放电做出了重要贡献。

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