首页> 外文期刊>Journal of Neurophysiology >Stimulation within the rostral ventrolateral medulla can evoke monosynaptic GABAergic IPSPs in sympathetic preganglionic neurons in vitro.
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Stimulation within the rostral ventrolateral medulla can evoke monosynaptic GABAergic IPSPs in sympathetic preganglionic neurons in vitro.

机译:延髓腹侧延髓内的刺激可在体外产生交感神经节前神经元中的单突触GABA能IPSP。

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摘要

The inhibitory responses of identified sympathetic preganglionic neurons (SPNs) to stimulation within the rostral ventrolateral medulla (RVLM) were studied to determine their nature and pharmacology. Whole cell patch-clamp recordings were made from 36 SPNs in the upper thoracic segments of the spinal cord in a neonatal rat brain stem-spinal cord preparation. Neurons were identified as SPNs on the basis of their antidromic activation after stimulation of the ipsilateral segmental ventral root and their morphology and location in the intermediolateral cell column and intercalated nucleus. In all SPNs, electrical stimulation of the RVLM evoked fast excitatory postsynaptic potentials (EPSPs) that were mediated by non-N-methyl-D-aspartate (NMDA) and NMDA receptors. These excitatory responses were the most prominent response in control artificial cerebrospinal fluid and have been studied previously. In 22 of the SPNs, RVLM stimulation also elicited fast inhibitory postsynaptic potentials (IPSPs), which increased in amplitude as the membrane was depolarized. Five of these neurons were not studied further as they responded occasionally with IPSPs that had highly variable onset latencies indicating the involvement of a polysynaptic pathway. In the remaining SPNs (n = 17), the evoked IPSPs persisted in the presence of the excitatory amino acid antagonists 6-cyano-7-nitroquinoxaline-2,3,-dione and D,L-2-amino-5-phosphonopentanoic acid. In eight of these SPNs, it was necessary to block the EPSPs to reveal the IPSPs. In the 7 SPNs tested, the onset latencies of the IPSPs were not significantly different from the onset latencies of the fast EPSPs. The low sweep-to-sweep fluctuations in onset latency of individual IPSPs (absolute average deviation: 0.4 ms) indicated that the IPSPs were elicited by activation of a monosynaptic pathway. The amplitudes of the IPSPs decreased in amplitude as the membrane was hyperpolarized and reversed in polarity at -70.3 +/- 1.7 mV (mean +/- SD), which was close to the equilibrium potential for chloride ions. In addition, in seven SPNs, bath applications of 5 microM bicuculline, a gamma-aminobuturic acid-A (GABAA) antagonist, abolished or reduced the evoked IPSPs. Five SPNs also were studied that displayed ongoing IPSPs. The amplitudes of these IPSPs increased with membrane depolarization and were blocked by bath applications of 5 microM bicuculline, suggesting that they also were mediated by activation of GABAA receptors. These results demonstrate the existence of a bulbospinal GABAergic pathway impinging directly onto SPNs. This pathway may be tonically active in the neonatal rat brain stem-spinal cord preparation.
机译:研究了已确定的交感神经节前神经元(SPNs)对延髓腹侧延髓(RVLM)内刺激的抑制反应,以确定其性质和药理作用。在新生大鼠脑干-脊髓制备物中,从脊髓上胸段的36个SPN进行全细胞膜片钳记录。根据神经元在刺激同侧节段腹根后的抗蠕动激活以及它们在形态学和在中间外侧细胞柱和插入核中的位置,被确定为SPN。在所有SPN中,对RVLM的电刺激都引起了由非N-甲基-D-天门冬氨酸(NMDA)和NMDA受体介导的快速兴奋性突触后电位(EPSP)。这些兴奋性反应是对照人工脑脊液中最突出的反应,并且先前已经进行了研究。在22个SPN中,RVLM刺激还引起快速抑制性突触后电位(IPSP),其在膜去极化时幅度增加。这些神经元中的五个没有被进一步研究,因为它们偶尔会与IPSPs反应,IPSPs具有较高的发作潜伏期,表明参与了多突触途径。在其余的SPN中(n = 17),诱发的IPSP在存在兴奋性氨基酸拮抗剂6-氰基-7-硝基喹喔啉-2,3,-二酮和D,L-2-氨基-5-膦基戊酸的情况下持续存在。 。在这些SPN中的八个中,有必要阻止EPSP以显示IPSP。在测试的7个SPN中,IPSP的开始延迟与快速EPSP的开始延迟没有显着差异。各个IPSP发作潜伏期的低扫掠波动(绝对平均偏差:0.4 ms)表明IPSP是由单突触途径的激活引起的。 IPSPs的振幅随着膜的超极化而减小,其极性在-70.3 +/- 1.7 mV(平均值+/- SD)下反转,这接近氯离子的平衡电位。此外,在七个SPN中,5 microM双瓜氨酸(一种γ-氨基丁酸-A(GABAA)拮抗剂)的沐浴应用废除了或减少了诱发的IPSP。还研究了五个显示正在进行的IPSP的SPN。这些IPSP的幅度随膜去极化而增加,并被5 microM双小分子的浴液阻滞,表明它们也受GABAA受体激活的介导。这些结果表明存在直接影响SPN的球根GABA能通路。该途径在新生大鼠脑干-脊髓制备中可能具有调性作用。

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