Pais Isabel, Hormuzdi Sheriar G, Monyer Hannah, Traub Roger D, Wood Ian C, Buhl Eberhard H, Whittington Miles A, LeBeau Fiona E N
School of Biomedical Sciences, University of Leeds, Leeds LS2 9NQ, United Kingdom.
J Neurophysiol. 2003 Apr;89(4):2046-54. doi: 10.1152/jn.00549.2002.
Bath application of kainate (100-300 nM) induced a persistent gamma-frequency (30-80 Hz) oscillation that could be recorded in stratum radiatum of the CA3 region in vitro. We have previously described that in knockout mice lacking the gap junction protein connexin 36 (Cx36KO), gamma-frequency oscillations are reduced but still present. We now demonstrate that in the Cx36KO mice, but not in wild-type (WT), large population field excitatory postsynaptic potentials, or sharp wave-burst discharges, also occurred during the on-going gamma-frequency oscillation. These spontaneous burst discharges were not seen in WT mice. Burst discharges in the Cx36KO mice occurred with a mean frequency of 0.23 +/- 0.11 Hz and were accompanied by a series of fast (approximately 60-115 Hz) population spikes or "ripple" oscillations in many recordings. Intracellular recordings from CA3 pyramidal cells showed that the burst discharges consisted of a depolarizing response and presumed coupling potentials (spikelets) could occasionally be seen either before or during the burst discharge. The burst discharges occurring in Cx36KO mice were sensitive to gap junctions blockers as they were fully abolished by carbenoxolone (200 microM). In control mice we made several attempts to replicate this pattern of sharp wave activity/ripples occurring with the on-going kainate-evoked gamma-frequency oscillation by manipulating synaptic and electrical signaling. Partial disruption of inhibition, in control slices, by bath application of the gamma-aminobutyric acid-A (GABA(A)) receptor antagonist bicuculline (1-4 microM) completely abolished all gamma-frequency activity before any burst discharges occurred. Increasing the number of open gap junctions in control slices by using trimethylamine (TMA; 2-10 mM), in conjunction with kainate, failed to elicit any sharp wave bursts or fast ripples. However, bath application of the potassium channel blocker 4-aminopyridine (4-AP; 20-80 microM) produced a pattern of activity in control mice (13/16 slices), consisting of burst discharges occurring in conjunction with kainate-evoked gamma-frequency oscillations, that was similar to that seen in Cx36KO mice. In a few cases (n = 9) the burst discharges were accompanied by fast ripple oscillations. Carbenoxolone also fully blocked the 4-AP-evoked burst discharges (n = 5). Our results show that disruption of electrical signaling in the interneuronal network can, in the presence of kainate, lead to the spontaneous generation of sharp wave/ripple activity similar to that observed in vivo. This suggests a complex role for electrically coupled interneurons in the generation of hippocampal network activity.
在体外,向CA3区辐射层施加100 - 300 nM的红藻氨酸可诱导持续的γ频率(30 - 80 Hz)振荡。我们之前曾描述过,在缺乏缝隙连接蛋白连接蛋白36的基因敲除小鼠(Cx36KO)中,γ频率振荡虽有所降低但仍然存在。我们现在证明,在Cx36KO小鼠中,而非野生型(WT)小鼠中,在持续的γ频率振荡期间还会出现大量群体场兴奋性突触后电位或尖波 - 爆发放电。这些自发爆发放电在WT小鼠中未观察到。Cx36KO小鼠中的爆发放电平均频率为0.23±0.11 Hz,并且在许多记录中伴随着一系列快速(约60 - 115 Hz)的群体锋电位或“涟漪”振荡。对CA3锥体细胞的细胞内记录显示,爆发放电由去极化反应组成,并且在爆发放电之前或期间偶尔可以看到推测的耦合电位(小锋电位)。Cx36KO小鼠中出现的爆发放电对缝隙连接阻滞剂敏感,因为它们被羧苄青霉素(200 μM)完全消除。在对照小鼠中,我们多次尝试通过操纵突触和电信号来复制这种与持续的红藻氨酸诱发的γ频率振荡同时出现的尖波活动/涟漪模式。在对照切片中,通过向浴槽中施加γ-氨基丁酸 - A(GABA(A))受体拮抗剂荷包牡丹碱(1 - 4 μM)部分破坏抑制作用,在任何爆发放电出现之前完全消除了所有γ频率活动。通过使用三甲胺(TMA;2 - 10 mM)与红藻氨酸联合使用来增加对照切片中开放缝隙连接的数量,未能引发任何尖波爆发或快速涟漪。然而,向浴槽中施加钾通道阻滞剂4 - 氨基吡啶(4 - AP;20 - 80 μM)在对照小鼠(13/16切片)中产生了一种活动模式,包括与红藻氨酸诱发的γ频率振荡同时出现的爆发放电,这与在Cx36KO小鼠中看到的相似。在少数情况下(n = 9),爆发放电伴随着快速涟漪振荡。羧苄青霉素也完全阻断了4 - AP诱发的爆发放电(n = 5)。我们的结果表明,在存在红藻氨酸的情况下,中间神经元网络中电信号的破坏可导致类似于体内观察到的尖波/涟漪活动的自发产生。这表明电耦合中间神经元在海马网络活动的产生中具有复杂的作用。
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