Cell Calcium Extrusion Systems and their Role in Epileptogenesis~!2009-05-14~!2010-01-06~!2010-04-21~!

Jorge Bravo-Martínez, B. Delgado-Coello, J. Mas-Oliva
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引用次数: 4

Abstract

The precise control for maintenance of a normal intracellular calcium concentration in eukaryote cells is ac- complished by several systems located at the plasma membrane, as well as several internal membrane systems. Neurons are especially sensitive to changes in these control systems, since when fail and calcium homeostasis disturbed, the cell's metabolism is immediately modified and a pathological condition emerges. Such a condition has been associated with epi- leptogenesis, and especially to those mechanisms associated to calcium entrance or ON mechanisms. On the other hand, calcium extrusion mechanisms or OFF mechanisms, have been investigated to a lesser extent and therefore remain much less understood. Here, we present a review of these calcium extrusion systems located at the plasma membrane considered to be critical in the process of epileptogenesis; first of all the plasma membrane calcium ATPase (PMCA) as the catalytic moiety of the enzyme that moves calcium outwards in an energy-dependent fashion, and the Na + /Ca 2+ exchanger (NCX) coupled to the (Na + /K + )-ATPase. Based on present knowledge considering the wide range of isoforms found for PMCA and NCX and their specific kinetic characteristics, a hypothesis for their participation on the OFF mechanisms related to the genesis of epilepsy is discussed. Epilepsy can be defined as a chronic illness of diverse etiology characterized by recurrent crises due to an excessive and synchronic burden of cerebral neurons, eventually asso- ciated with diverse clinical and paraclinical manifestations. Epilepsy is a common pathology; World Health Organiza- tion (WHO) statistics revealed in the year of 2001 a preva- lence of 8.2 per 1,000 individuals in developed countries and 10 per 1,000 in developing countries. During the same year, incidence in developed countries was 50 per 100,000 indi- viduals in the general population, and 100 per 100,000 in developing countries. The analysis we have performed in the present study is related to the 50% of these patients that pre- sent by diverse external causes an acquired epilepsy (1). One very important period of epilepsy comprises epileptogenesis, i.e., the period in which epilepsy is developed, which can be considered the period between the lesion and the appearance of clinical manifestations. Epileptogenesis includes all phe- nomena that induce normal cells to discharge abnormally, which when repeated in a continuous fashion, produce an epileptic focus. For these phenomena to be expressed in cells, a change is required in the majority of systems control- ling neuronal excitability and inhibitory processes. Such phenomena allow an exaggerated abnormal discharge of neurons provoking hyperexcitability in the long term. During the period of epileptogenesis, there also appear aberrant in- terconnections that promote neuronal synchronization with the consequent clinical manifestations (1).
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细胞钙挤压系统及其在癫痫发生中的作用2009-05-14 2010-01-06 2010-04-21
在真核生物细胞中,维持正常的细胞内钙浓度的精确控制是由位于质膜上的几个系统以及几个内膜系统完成的。神经元对这些控制系统的变化特别敏感,因为当失败和钙稳态被扰乱时,细胞的代谢立即被改变,并出现病理状态。这种情况与外睑下垂发生有关,特别是与钙进入或ON机制有关的机制。另一方面,钙挤压机制或OFF机制的研究程度较低,因此仍然知之甚少。在这里,我们介绍了这些钙挤压系统位于质膜被认为是癫痫发生过程中的关键;首先,质膜钙atp酶(PMCA)作为酶的催化部分,以能量依赖的方式将钙向外移动,并且Na + / ca2 +交换器(NCX)偶联到(Na + /K +)- atp酶。基于现有的知识,考虑到PMCA和NCX广泛的同工异构体及其特定的动力学特征,讨论了它们参与癫痫发生相关的OFF机制的假设。癫痫可以被定义为一种多种病因的慢性疾病,其特征是由于大脑神经元的过度和同步负担而反复发作,最终与多种临床和临床旁表现相关。癫痫是一种常见的病理;世界卫生组织(卫生组织)的统计数字显示,2001年,发达国家每1 000人中有8.2人患此病,发展中国家每1 000人中有10人患此病。同年,发达国家的发病率为每10万人中有50人,发展中国家为每10万人中有100人。我们在本研究中所做的分析与50%的这些患者有关,这些患者由各种外部原因表现为获得性癫痫(1)。癫痫的一个非常重要的时期包括癫痫发生,即癫痫发展的时期,可以认为是从病变到出现临床表现之间的时期。癫痫发生包括所有诱导正常细胞异常放电的现象,当这种现象以连续的方式重复时,产生癫痫灶。为了使这些现象在细胞中表达,需要在控制神经元兴奋性和抑制过程的大多数系统中发生变化。这种现象使得神经元的异常放电在长期内会引起过度兴奋。在癫痫发生期间,也会出现异常的连接,促进神经元同步,从而产生临床表现(1)。
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