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锂对突触体钙通量的影响。

Effects of lithium on synaptosomal Ca2+ fluxes.

作者信息

Koenig M L, Jope R S

机构信息

Department of Pharmacology, University of Alabama, Birmingham 35294.

出版信息

Psychopharmacology (Berl). 1988;96(2):267-72. doi: 10.1007/BF00177573.

Abstract

Lithium is the primary treatment for mania, and it has been employed as a therapeutic agent in the treatment of a number of other conditions. In spite of its widespread clinical use, the specific mechanism by which lithium acts is still not known. Because lithium bears some chemical resemblance to Ca2+ and because it has been found to interfere with many Ca2+-dependent processes, we investigated the possibility that lithium can alter intracellular Ca2+ homeostasis by an effect on Ca2+ fluxes. When added in vitro to synaptosomes prepared from rat forebrains, lithium had no effect on 45Ca2+ influx mediated by fast or slow phase depolarization-dependent Ca2+ channels or by Na+/Ca2+ exchange. In vitro treatment with lithium also had no effect on ATP-dependent Ca2+ sequestration by mitochondria or synaptosomal endoplasmic reticulum. In contrast, 45Ca2+ influx in synaptosomes prepared from rats treated chronically with lithium was increased significantly relative to controls. The fact that chronic in vivo treatment with lithium affected synaptosomal Ca2+ flux whereas in vitro treatment did not is consistent with the time course of therapeutic effectiveness in man. The results suggest that lithium does not directly interact with synaptosomal Ca2+ flux, but rather may influence Ca2+ flux through an indirect mechanism following chronic treatment.

摘要

锂是治疗躁狂症的主要药物,它还被用作治疗许多其他病症的治疗剂。尽管锂在临床上广泛使用,但其作用的具体机制仍不清楚。由于锂在化学性质上与Ca2+有一些相似之处,并且已发现它会干扰许多依赖Ca2+的过程,因此我们研究了锂是否可以通过影响Ca2+通量来改变细胞内Ca2+稳态的可能性。当在体外添加到从大鼠前脑制备的突触体中时,锂对由快速或缓慢相去极化依赖性Ca2+通道或Na+/Ca2+交换介导的45Ca2+内流没有影响。锂的体外处理对线粒体或突触体内质网的ATP依赖性Ca2+螯合也没有影响。相比之下,与对照组相比,长期用锂处理的大鼠制备的突触体中的45Ca2+内流显著增加。长期体内锂治疗影响突触体Ca2+通量而体外治疗不影响这一事实与人类治疗效果的时间进程一致。结果表明,锂不直接与突触体Ca2+通量相互作用,而是可能在长期治疗后通过间接机制影响Ca2+通量。

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