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首页> 外文期刊>The Journal of Physiology >Carbenoxolone blockade of neuronal network activity in culture is not mediated by an action on gap junctions.
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Carbenoxolone blockade of neuronal network activity in culture is not mediated by an action on gap junctions.

机译:羧甲基环己酮对培养物中神经元网络活性的阻断作用不是通过对间隙连接的作用来介导的。

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Spontaneous activity in the central nervous system is strongly suppressed by blockers of gap junctions (GJs), suggesting that GJs contribute to network activity. However, the lack of selective GJ blockers prohibits the determination of their site of action, i.e. neuronal versus glial. Astrocytes are strongly coupled through GJs and have recently been shown to modulate synaptic transmission, yet their role in neuronal network activity was not analysed. The present study investigated the effects and site of action of the GJ blocker, carbenoxolone (CBX), on neuronal network activity. To this end, we used cultures of hippocampal or cortical neurons, plated on astrocytes. In these cultures neurons display spontaneous synchronous activity and GJs are found only in astrocytes. CBX induced in these neurons a reversible suppression of spontaneous action potential discharges, synaptic currents and synchronised calcium oscillations. Moreover, CBX inhibited oscillatory activity induced by the GABAA antagonist, bicuculline. These effects were not due to blockade of astrocytic GJs, since they were not mimicked nor occluded by endothelin-1 (ET-1), a peptide known to block astrocytic GJs. Also, these effects were still present in co-cultures of wild-type neurons plated on astrocytes originating from connexin-43 (Cx43) knockout mice, and in neuronal cultures which contain few isolated astrocytes. CBX was not likely to exert its effect through neuronal GJs either, as immunostaining for major neuronal connexins (Cx) as well as dye or electrical coupling, were not detected in the different models of cultured neurons examined. Finally while CBX (at 100 microM) did not modify presynaptic transmitter release and postsynaptic responses to glutamate, it did cause an increase in the action potential threshold and strongly decreased the firing rate in response to a sustained depolarising current. These data demonstrate that CBX does not exert its action on network activity of cultured neurons through astrocytic GJs and suggest that it has direct effects on neurons, not involving GJs.
机译:间隙连接(GJs)的阻滞剂强烈抑制中枢神经系统中的自发活动,表明GJ有助于网络活动。但是,由于缺乏选择性的GJ阻滞剂,无法确定其作用部位,即神经元与神经胶质。星形胶质细胞通过GJs强烈耦合,最近已显示出可调节突触传递,但尚未分析它们在神经元网络活动中的作用。本研究调查了GJ阻断剂羧苄索隆(CBX)对神经元网络活动的影响和作用部位。为此,我们使用了铺在星形胶质细胞上的海马或皮质神经元培养物。在这些培养物中,神经元显示出自发的同步活动,仅在星形胶质细胞中发现GJ。 CBX在这些神经元中诱导自发动作电位放电,突触电流和同步钙振荡的可逆抑制。此外,CBX抑制了由GABAA拮抗剂双小茴香碱诱导的振荡活性。这些作用不是由于星形胶质细胞GJ的阻断,因为它们并未被内皮素-1(ET-1)(一种可阻断星形胶质细胞GJ的肽)模拟或封闭。同样,这些作用仍然存在于接种于连接蛋白43(Cx43)基因敲除小鼠的星形胶质细胞上的野生型神经元的共培养物中,以及在含有少量分离的星形胶质细胞的神经元培养物中。 CBX也不太可能通过神经元GJ发挥作用,因为在所研究的培养神经元的不同模型中均未检测到主要神经元连接蛋白(Cx)的免疫染色以及染料或电耦合。最后,尽管CBX(在100 microM下)没有改变突触前递质的释放和对谷氨酸的突触后反应,但确实引起动作电位阈值的增加,并响应持续的去极化电流而大大降低了发射速率。这些数据表明,CBX不会通过星形胶质细胞GJ对培养的神经元的网络活动发挥作用,并且表明它对神经元具有直接作用,而并不涉及GJ。

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