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血清素会增加大鼠深层背角神经元中初级传入诱发的长时程抑制的发生率。

Serotonin increases the incidence of primary afferent-evoked long-term depression in rat deep dorsal horn neurons.

作者信息

Garraway S M, Hochman S

机构信息

Department of Physiology, University of Manitoba, Winnipeg, Manitoba R3E 0W3, Canada.

出版信息

J Neurophysiol. 2001 May;85(5):1864-72. doi: 10.1152/jn.2001.85.5.1864.

DOI:10.1152/jn.2001.85.5.1864
PMID:11353003
Abstract

5-hydroxytryptamine (5-HT) is released in spinal cord by descending systems that modulate somatosensory transmission and can potently depress primary afferent-evoked synaptic responses in dorsal horn neurons. Since primary afferent activity-induced long-term potentiation (LTP) may contribute to central sensitization of nociception, we studied the effects of 5-HT on the expression of sensory-evoked LTP and long-term depression (LTD) in deep dorsal horn (DDH) neurons. Whole cell, predominantly current clamp, recordings were obtained from DDH neurons in transverse slices of neonatal rat lumbar spinal cord. The effect of 5-HT on dorsal-root stimulation-evoked synaptic responses was tested before, during, or after high-frequency conditioning stimulation (CS). In most cells (80%), 5-HT caused a depression of the naïve synaptic response. Even though 5-HT depressed evoked responses, CS in the presence of 5-HT was not only still capable of inducing LTD but also increased its incidence from 54% in controls to 88% (P < 0.001). Activation of ligands selective for 5-HT(1A/1B) and 5-HT(1B), but not 5-HT(2A/2C) or 5-HT(3) receptors, best reproduced these actions. 5-HT also potently depressed postconditioning synaptic responses regardless of whether the induced plasticity was LTP or LTD. Our results demonstrate that in addition to depressing the amplitude of evoked sensory input, 5-HT can also control the direction of its long-term modifiability, favoring the expression of LTD. These findings demonstrate cellular mechanisms that may contribute to the descending serotonergic control of nociception.

摘要

5-羟色胺(5-HT)由调节体感传递的下行系统释放到脊髓中,并且能够有效地抑制背角神经元中初级传入神经诱发的突触反应。由于初级传入神经活动诱导的长时程增强(LTP)可能促成伤害性感受的中枢敏化,因此我们研究了5-HT对深部背角(DDH)神经元中感觉诱发LTP和长时程抑制(LTD)表达的影响。采用全细胞记录,主要是电流钳记录,从新生大鼠腰段脊髓横切片中的DDH神经元获取数据。在高频条件刺激(CS)之前、期间或之后,测试5-HT对背根刺激诱发的突触反应的影响。在大多数细胞(80%)中,5-HT导致原始突触反应受到抑制。尽管5-HT抑制了诱发反应,但在存在5-HT的情况下进行CS不仅仍然能够诱导LTD,而且将其发生率从对照组的54%提高到了88%(P < 0.001)。对5-HT(1A/1B)和5-HT(1B)有选择性的配体激活,但对5-HT(2A/2C)或5-HT(3)受体无激活作用,最能重现这些作用。无论诱导的可塑性是LTP还是LTD,5-HT也能有效地抑制条件刺激后的突触反应。我们的结果表明,除了抑制诱发的感觉输入幅度外,5-HT还可以控制其长期可塑性的方向,有利于LTD的表达。这些发现揭示了可能有助于下行5-羟色胺能对伤害性感受进行控制的细胞机制。

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