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通过螯合重金属对大鼠海马中胆囊收缩素浓度的调节

Modulation of cholecystokinin concentrations in the rat hippocampus by chelation of heavy metals.

作者信息

Stengaard-Pedersen K, Larsson L I, Fredens K, Rehfeld J F

出版信息

Proc Natl Acad Sci U S A. 1984 Sep;81(18):5876-80. doi: 10.1073/pnas.81.18.5876.

Abstract

Previously, we have reported that enkephalins, cholecystokinin, and heavy metals show roughly parallel distributional patterns in the hippocampus. A substantial body of evidence indicates that cholecystokinin-octapeptide (CCK-8) and enkephalins act as neurotransmitters. A CCK-8 degrading enzyme was recently detected in brain synaptosomes. Its activity depended on free thiol groups and the presence of a heavy metal. Since the heavy metal-containing neuropil is closely related to CCK-immunoreactive nerve terminals, we have investigated the effect of metal chelation on CCK components in the rat hippocampus. In vivo treatment of rats with a single dose of the chelating agent diethyldithiocarbamate caused a reversible chelation of heavy metals in the hippocampus. This effect was paralleled by a 3-fold increase in hippocampal content of CCK-8 and a smaller increase in the intermediate forms of CCK (CCK-58, CCK-39, CCK-33). Diethyldithiocarbamate also decreased the spontaneous motility and aggressiveness of the rats. These data show reversible changes of neuronal CCK processing by a drug, and hence they provide additional evidence that CCK is involved in the regulation of neuronal activities.

摘要

此前,我们曾报道脑啡肽、胆囊收缩素和重金属在海马体中呈现大致平行的分布模式。大量证据表明,胆囊收缩素八肽(CCK-8)和脑啡肽作为神经递质发挥作用。最近在脑突触体中检测到一种CCK-8降解酶。其活性依赖于游离巯基和重金属的存在。由于含重金属的神经纤维网与CCK免疫反应性神经末梢密切相关,我们研究了金属螯合对大鼠海马体中CCK成分的影响。用螯合剂二乙基二硫代氨基甲酸盐对大鼠进行单次体内治疗,可导致海马体中重金属的可逆螯合。这种效应伴随着CCK-8海马体含量增加3倍,以及CCK中间形式(CCK-58、CCK-39、CCK-33)的较小增加。二乙基二硫代氨基甲酸盐还降低了大鼠的自发运动能力和攻击性。这些数据显示了药物对神经元CCK加工的可逆变化,因此它们提供了额外的证据,证明CCK参与神经元活动的调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6e13/391815/9b0a19ee687e/pnas00619-0261-a.jpg

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