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海马乙酰胆碱释放的调节:白细胞介素-2的一种强效中枢作用。

Modulation of hippocampal acetylcholine release: a potent central action of interleukin-2.

作者信息

Hanisch U K, Seto D, Quirion R

机构信息

Douglas Hospital Research Centre, Department of Psychiatry, Montreal, Québec, Canada.

出版信息

J Neurosci. 1993 Aug;13(8):3368-74. doi: 10.1523/JNEUROSCI.13-08-03368.1993.

DOI:10.1523/JNEUROSCI.13-08-03368.1993
PMID:8340813
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6576518/
Abstract

The potential of the T-cell growth factor interleukin-2 (IL-2) to modulate the release of ACh from rat hippocampus was studied in vitro, as a means to investigate the possible functional significance of this cytokine in the CNS. Hippocampal slices were superfused with Krebs' buffer medium, and endogenous ACh released into the superfusate was measured using a radioenzymatic assay. Recombinant human IL-2 present during a stimulation with 25 mM KCl altered, in a concentration-dependent manner, the evoked transmitter release. At a concentration of 15 U/ml (< or = 1 nM), IL-2 inhibited ACh release by more than 50% of the control level (evoked ACh release from the untreated contralateral hemispheres). Inhibition was observed within 20 min of tissue exposure to IL-2 and lasted for up to 1 hr. The inhibitory effect of IL-2 was reversible since transient tissue exposure to IL-2 did not affect subsequent evoked ACh release. IL-2 at this concentration also significantly decreased evoked ACh in frontal cortical slices, but was ineffective in the parietal cortex and striatum, revealing that IL-2 selectively modulates the release of ACh from certain, but not all, cholinergic nerve terminals in the CNS. At very low concentrations (1.5 mU/ml, < or = 0.1 pM), IL-2 transiently increased hippocampal evoked ACh release, resulting in a biphasic dose-response profile with no significant effect observed at 0.015 mU/ml (< or = 1 fM). Other cytokines (IL-1 alpha, IL-3, IL-5, IL-6, interferon alpha), tested in hippocampal slice incubations, failed to modulate ACh release.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

作为研究这种细胞因子在中枢神经系统中可能的功能意义的一种手段,我们在体外研究了T细胞生长因子白细胞介素-2(IL-2)调节大鼠海马中乙酰胆碱(ACh)释放的潜力。用 Krebs 缓冲液培养基对海马切片进行灌流,并使用放射酶法测定释放到灌流液中的内源性 ACh。在 25 mM KCl 刺激期间存在的重组人 IL-2 以浓度依赖性方式改变了诱发的递质释放。在浓度为 15 U/ml(≤1 nM)时,IL-2 将 ACh 释放抑制至对照水平(从未经处理的对侧半球诱发的 ACh 释放)的 50%以上。在组织暴露于 IL-2 的 20 分钟内观察到抑制作用,并持续长达 1 小时。IL-2 的抑制作用是可逆的,因为短暂的组织暴露于 IL-2 并不影响随后诱发的 ACh 释放。该浓度的 IL-2 也显著降低了额叶皮质切片中诱发的 ACh,但在顶叶皮质和纹状体中无效,这表明 IL-2 选择性地调节中枢神经系统中某些但不是所有胆碱能神经末梢的 ACh 释放。在非常低的浓度(1.5 mU/ml,≤0.1 pM)下,IL-2 短暂增加海马诱发的 ACh 释放,导致双相剂量反应曲线,在 0.015 mU/ml(≤1 fM)时未观察到显著影响。在海马切片培养中测试的其他细胞因子(IL-1α、IL-3、IL-5、IL-6、干扰素α)未能调节 ACh 释放。(摘要截短至 250 字)

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