首页> 外文期刊>The Journal of Physiology >Short-term facilitation evoked during brief afferent tetani is not altered by long-term potentiation in the guinea-pig hippocampal CA1 region.
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Short-term facilitation evoked during brief afferent tetani is not altered by long-term potentiation in the guinea-pig hippocampal CA1 region.

机译:豚鼠海马CA1区的长期增强作用不会改变短暂传入破伤风期间引起的短期促进作用。

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1. The aim was to examine whether long-term potentiation (LTP) had effects on short-term synaptic plasticity outside those predicted from its effect on single volley-induced responses. Field recordings from the CA1 region of guinea-pig hippocampal slices were used, and short- term plasticity was evoked by five-impulse trains of 20 and 50 Hz. 2. The five-impulse trains were evoked in the presence of D(-)-2-amino-5-phosphonopentanoic acid (D-AP5; 20-50 microM), picrotoxin (100 microM), and 2-OH-saclofen (200 microM), and care was taken to avoid initiation of postsynaptic spike activation. Field responses were thus considered to reflect non-NMDA receptor-mediated activity only, and demonstrated a net facilitation during the trains. 3. The facilitation was found, on average, to be unaffected by LTP, evoked by strong afferent tetanization. This was true also when release probability had been altered either by the adenosine agonist N-cyclohexyladenosine (CHA; 100 nM) or the antagonist 8-cyclopentyl-1,3-dipropylxanthine (DPCPX; 200 nM). When examined for individual experiments, cases with increases, or decreases, of facilitation following LTP were observed. These deviations showed no relation to initial release probability or to LTP magnitude, and they were also observed in control inputs not subjected to LTP. 4. Impairment of non-NMDA receptor desensitization by cyclothiazide (30 microM) increased facilitation observed during a 50 Hz, but not a 20 Hz, train. LTP had no effect on facilitation, in the presence of this drug, either during 20 or 50 Hz trains. 5. The results suggest that the effect of LTP in the hippocampal CA1 region on non-NMDA receptor-mediated synaptic responses to a brief afferent tetanus does not differ from that on a low-frequency, single volley-induced response. They do not support the notion that LTP is based on changes in release probability of previously active synapses. If LTP is based on recruitment of previously, pre- or postsynaptically, silent synapses, these synapses must have, on average, release characteristics similar to the previously active ones.
机译:1.目的是研究长期增强(LTP)是否对短期突触可塑性产生影响,但其对单次凌空诱发反应的影响尚不能预测。使用了豚鼠海马切片CA1区的现场记录,并通过20和50 Hz的五脉冲序列诱发了短期可塑性。 2.在D(-)-2-氨基-5-膦基戊酸(D-AP5; 20-50 microM),微毒素(100 microM)和2-OH-沙氯芬( 200 microM),并注意避免引发突触后突波激活。因此,场响应被认为仅反映了非NMDA受体介导的活性,并在训练过程中显示出净的促进作用。 3.平均而言,发现便利化不受LTP的影响,而强烈的传入tétanization引起了这种促进。当通过腺苷激动剂N-环己基腺苷(CHA; 100 nM)或拮抗剂8-环戊基-1,3-二丙基黄嘌呤(DPCPX; 200 nM)改变释放可能性时,也是如此。当检查单个实验时,观察到LTP后促进程度增加或减少的情况。这些偏差与初始释放概率或LTP大小无关,在未接受LTP的对照输入中也观察到了。 4.环噻嗪(30 microM)对非NMDA受体脱敏的损害增加了在50 Hz而不是20 Hz的训练过程中的促进作用。在20或50 Hz的频率下,存在该药时,LTP对促进作用没有影响。 5.结果表明,海马CA1区的LTP对短暂传入破伤风的非NMDA受体介导的突触反应的影响与低频,一次截击诱导的反应的影响没有区别。他们不支持LTP基于先前活动的突触释放概率变化的观点。如果LTP基于先前,突触前或突触后沉默突触的募集,则这些突触的平均释放特性必须类似于先前活跃的突触。

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