Jones R S, Lambert J D
Division of Neuroscience, John Curtin School of Medical Research, Australian National University, Canberra, ACT.
Neuroscience. 1990;34(3):657-70. doi: 10.1016/0306-4522(90)90172-z.
A slice preparation was used to study the spread of epileptiform activity in the rat entorhinal cortex. Interictal-like discharges were induced in the medial entorhinal cortex by blocking synaptic inhibition mediated via GABAA-receptors. Recorded intracellularly, these discharges consisted of an initial paroxysmal depolarizing shift followed by a variable number of afterdischarges. There was no apparent difference between these events whether they were recorded in isolated cortical slices or in slices where the hippocampus and subicular complex remained attached. The events were also unaffected by droplets of a xylocaine solution applied to sites in the hippocampus, subicular complex or superficial layers of the entorhinal cortex but applications to layer IV/V, lateral or medial to the recording site could reduce the number of afterdischarges without affecting the initial paroxysmal shift. Simultaneous intracellular recordings from neurons in layer IV/V and layer II of the medial entorhinal cortex showed that the paroxysmal depolarizing shift and all afterdischarges in the deeper layer always preceded those recorded in the superficial layer, and these events invariably occurred on a one-to-one basis. This was true whether the events were evoked or occurred spontaneously. The delay varied between 2 and 11 ms but was consistent for a given cell pair. A similar relationship existed between discharges recorded simultaneously in layer IV/V neurons and layer VI neurons, events in the layer IV/V cells preceding those in the deeper layer. Discharges recorded simultaneously in pairs of layer IV/V neurons showed more complex relationships. Paroxysmal depolarizing shifts were always recorded in both cells and the discharge could occur at the more medial site before the more lateral, or vice versa. For a given pair the temporal relationship was invariable. It was often the case, however, that the temporal relationship between afterdischarges was reversed with respect to the initial paroxysmal shift. This relationship was also invariable in a given pair of cells. Interictal-like discharges in layers II or IV/V neurons could be abolished by perfusion with 6-cyano-7-nitro-quinoxaline-2,3-dione which is an antagonist for the non-N-methyl-D-aspartate (i.e. quisqualate/kainate) subtype of excitatory amino acid receptor. The afterdischarges associated with the events were abolished in an all-or-none fashion whereas the blockade of the paroxysmal depolarizing shift was progressive. Antagonists of N-methyl-D-aspartate receptors also abolished afterdischarges but only reduced the initial paroxysmal shift. It is concluded that the interictal-like discharges arise intrinsically within the cortex and are not influenced by input from hippocampal or subicular structures.(ABSTRACT TRUNCATED AT 400 WORDS)
采用脑片制备技术研究癫痫样活动在大鼠内嗅皮层的传播。通过阻断由GABAA受体介导的突触抑制,在内侧内嗅皮层诱发类发作间期放电。细胞内记录显示,这些放电由最初的阵发性去极化偏移及随后数量不等的后放电组成。无论在分离的皮层脑片还是海马和下托复合体仍相连的脑片中记录这些事件,均无明显差异。这些事件也不受施加于海马、下托复合体或内嗅皮层表层部位的利多卡因溶液滴的影响,但施加于记录部位外侧或内侧的IV/V层可减少后放电数量,而不影响最初的阵发性偏移。内侧内嗅皮层IV/V层和II层神经元的同步细胞内记录显示,深层的阵发性去极化偏移和所有后放电总是先于表层记录到的相应事件,且这些事件总是一对一发生。无论这些事件是诱发的还是自发的,都是如此。延迟时间在2至1l毫秒之间变化,但对给定的细胞对而言是一致的。IV/V层神经元和VI层神经元同时记录的放电之间也存在类似关系,IV/V层细胞的事件先于深层细胞的事件。IV/V层神经元对同时记录的放电显示出更复杂的关系。两个细胞均记录到阵发性去极化偏移,放电可先在更内侧部位出现,然后在更外侧部位出现,反之亦然。对给定的细胞对而言时间关系是固定的。然而,后放电之间的时间关系相对于最初的阵发性偏移往往是相反的。在给定的细胞对中这种关系也是固定的。灌注6-氰基-7-硝基喹喔啉-2,3-二酮(一种兴奋性氨基酸受体的非N-甲基-D-天冬氨酸(即quisqualate/海人藻酸)亚型拮抗剂)可消除II层或IV/V层神经元的类发作间期放电。与这些事件相关的后放电以全或无的方式被消除,而阵发性去极化偏移的阻断是渐进性的。N-甲基-D-天冬氨酸受体拮抗剂也可消除后放电,但仅减少最初的阵发性偏移。结论是,类发作间期放电在皮层内源性产生,不受海马或下托结构输入的影响。(摘要截短于400字)
