Olney J W, Collins R C, Sloviter R S
Adv Neurol. 1986;44:857-77.
It is well established that the putative excitatory neurotransmitters, glutamate (Glu) and aspartate (Asp), are neurotoxins that have the potential of destroying central neurons by an excitatory mechanism. Kainic acid (KA), a rigid structural analog of Glu, powerfully reproduces the excitatory neurotoxic (excitotoxic) action of Glu on central neurons and, in addition, causes sustained limbic seizures and a pattern of seizure-linked brain damage in rats that closely resembles that observed in human epilepsy. In the course of studying the seizure-related brain damage syndrome induced by KA, we observed that a similar type of brain damage occurs as a consequence of sustained seizure activity induced by any of a variety of methods. These included intraamygdaloid or supradural administration of known convulsants such as bicuculline, picrotoxin and folic acid, or systemic administration of lithium and cholinergic agonists or cholinesterase inhibitors that have not commonly been viewed as convulsants. We have further observed that this type of brain damage can be reproduced in the hippocampus by persistent electrical stimulation of the perforant path, a major excitatory input to the hippocampus that is thought to use Glu as transmitter. It is a common feature of all such neurotoxic processes that the acute cytopathology resembles the excitotoxic type of damage induced by Glu or Asp, which is acute swelling of dendrites and vacuolar degeneration of neuronal soma, without acute changes in axons or axon terminals. We have found that the seizure-brain damage syndrome induced by cholinergic agents can be prevented by pretreatment with atropine and that the syndrome induced by any of the above methods, cholinergic or noncholinergic, can be either prevented or aborted respectively by either pre-or posttreatment with diazepam. Our findings in experimental animals may be summarized in terms of their potential relevance to human epilepsy as follows. Sustained complex partial seizure activity consistently results in cellular damage if allowed to continue for longer than 1 hr. Hippocampal, or Ammon's horn, sclerosis is the primary pathological result. It may be a priority goal, therefore, in the management of human epilepsy to control such seizure activity within very narrow limits. This proposal is discussed in terms of three major transmitter systems that may be involved; cholinergic, GABAergic, and glutamergic/aspartergic. The cholinergic system may play a role in generating or maintaining this type of seizure activity, and anticholinergics may protect against it provided they are given prior to commencement of behavioral seizures.(ABSTRACT TRUNCATED AT 400 WORDS)
公认的兴奋性神经递质谷氨酸(Glu)和天冬氨酸(Asp)是神经毒素,它们有可能通过兴奋性机制破坏中枢神经元。海人酸(KA)是Glu的一种刚性结构类似物,能有力地重现Glu对中枢神经元的兴奋性神经毒性(兴奋毒性)作用,此外,还会导致大鼠持续的边缘叶癫痫发作以及与人类癫痫中观察到的情况极为相似的癫痫相关脑损伤模式。在研究由KA诱导的癫痫相关脑损伤综合征的过程中,我们观察到,由多种方法诱导的持续癫痫活动会导致类似类型的脑损伤。这些方法包括在杏仁核内或硬脑膜上给予已知的惊厥剂,如荷包牡丹碱、印防己毒素和叶酸,或全身给予锂、胆碱能激动剂或胆碱酯酶抑制剂,这些通常不被视为惊厥剂。我们进一步观察到,通过持续电刺激穿通路径(海马的主要兴奋性输入,被认为以Glu作为递质),可以在海马中重现这种类型的脑损伤。所有这些神经毒性过程的一个共同特征是,急性细胞病理学类似于由Glu或Asp诱导的兴奋毒性损伤类型,即树突急性肿胀和神经元胞体空泡变性,而轴突或轴突终末没有急性变化。我们发现,胆碱能药物诱导的癫痫 - 脑损伤综合征可以通过用阿托品预处理来预防,并且上述任何方法(胆碱能或非胆碱能)诱导的综合征可以分别通过地西泮的预处理或后处理来预防或终止。我们在实验动物中的发现就其与人类癫痫的潜在相关性可总结如下。如果持续复杂部分性癫痫活动持续超过1小时,就会持续导致细胞损伤。海马或海马角硬化是主要的病理结果。因此,在人类癫痫的治疗中,将这种癫痫活动控制在非常狭窄的范围内可能是一个首要目标。该提议将根据可能涉及的三个主要递质系统进行讨论;胆碱能、GABA能和谷氨酸能/天冬氨酸能。胆碱能系统可能在产生或维持这种类型的癫痫活动中起作用,并且抗胆碱能药物如果在行为性癫痫发作开始之前给予,可能会起到保护作用。(摘要截取自400字)
