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首页> 外文期刊>Journal of Neurophysiology >Robust suppression of afferent-induced excitation in the rat spinal dorsal horn after conditioning low-frequency stimulation.
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Robust suppression of afferent-induced excitation in the rat spinal dorsal horn after conditioning low-frequency stimulation.

机译:调节低频刺激后,对大鼠脊髓背角传入刺激的抑制作用得到了强有力的抑制。

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The neuronal plasticity in the spinal dorsal horn induced after conditioning low-frequency stimulation of afferent A fibers, and its relationship with spinal inhibitory networks, was investigated with an optical-imaging method that detects neuronal excitation. High-intensity single-pulse stimulation of the dorsal root activating both A and C fibers evoked an optical response in the dorsal horn in transverse slices of 12- to 25-day-old rat spinal cords stained with a voltage-sensitive dye, RH-482. The optical response, reflecting the net excitation of neuronal elements along the thickness of each slice, was suppressed after a conditioning low-frequency stimulation (0.2-1 Hz for 10 min) to A fibers in the dorsal root. The degree of suppression was largest in the lamina II of the dorsal horn (48% reduction), where the majority of C fibers terminate, and much less in the deeper dorsal horn (5% reduction in laminae III-IV). The onset of suppression was somewhat slow; after the low-frequency stimulation, the magnitude of excitation gradually decreased, reached the maximum effect 30 min after the conditioning, and remained at the suppressed level for >1 h. Suppression was not observed when the low-frequency stimulation was given during a 20-min perfusion with a solution containing an NMDA-receptor antagonist, DL-2-amino-5-phosphonovaleric acid (30 microM). A brief application of an opioid-receptor antagonist, naloxone (0.5 microM), inhibited the induction, but not the maintenance, of low-frequency stimulus-induced suppression. However, treatments with the GABA(A) receptor antagonist bicuculline (1 microM) and the glycine receptor antagonist strychnine (0.3 microM) did not affect suppression induction and maintenance. In conclusion, conditioning low-frequency stimulation to A fibers interferes with the afferent-induced excitation in the dorsal horn. The low-frequency stimulation-induced suppression is maintained by a reduction of glutamatergic excitatory transmissions in the dorsal horn, not by an enhanced inhibition. Activation of the spinal opioid-mediated system by low-frequency stimulation, but not the inhibitory amino acid-mediated system, is necessary to initiate robust suppression. The long-term depression of afferent synaptic efficacy onto excitatory interneurons likely takes the primary role in the robust suppression of neuronal excitation in the dorsal horn.
机译:利用检测神经元兴奋的光学成像方法研究了对传入A纤维进行低频刺激后对脊髓背角的神经元可塑性的影响及其与脊髓抑制网络的关系。对背根的高强度单脉冲刺激同时激活了A和C纤维,在12至25天大的大鼠脊髓横切片中的背角中引起了光学响应,并用一种​​压敏染料RH- 482。在对背根中的A纤维进行低频调节(0.2-1 Hz,持续10分钟)后,抑制了沿着每个切片的厚度反射神经元元素净激发的光学响应。抑制程度最大的是在背角的椎板II中(减少48%),其中大部分C纤维终止,而在较深的背角中的抑制程度则要小得多(在III-IV层中减少5%)。压抑的发生有些缓慢;低频刺激后,激发的强度逐渐降低,在调理后30分钟达到最大作用,并保持在抑制水平> 1 h。在使用含有NMDA受体拮抗剂DL-2-氨基-5-膦酸戊酸(30 microM)的溶液灌注20分钟的过程中进行低频刺激时,未观察到抑制。阿片类药物受体拮抗剂纳洛酮(0.5 microM)的简短应用抑制了低频刺激诱导的抑制的诱导,但没有抑制。但是,用GABA(A)受体拮抗剂双瓜氨酸(1 microM)和甘氨酸受体拮抗剂士的宁(0.3 microM)进行的治疗不会影响抑制的诱导和维持。总之,调节低频刺激到A纤维会干扰背角传入的刺激。低频刺激诱导的抑制作用通过减少背角中的谷氨酸能兴奋性传递而得以维持,而不是通过增强的抑制作用来维持。通过低频刺激来激活脊髓阿片样物质介导的系统,而不是抑制性氨基酸介导的系统,是启动稳健抑制所必需的。长期抑制兴奋性神经元传入突触功效可能主要在强烈抑制背角神经元兴奋中起主要作用。

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