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基于离子依赖性和5-羟色胺敏感性对小鼠脑[3H]丙咪嗪结合的细分。

Subdivision of mouse brain [3H]imipramine binding based on ion dependence and serotonin sensitivity.

作者信息

Severson J A, Woodward J J, Wilcox R E

出版信息

J Neurochem. 1986 Jun;46(6):1743-54. doi: 10.1111/j.1471-4159.1986.tb08492.x.

Abstract

The specific binding of [3H]imipramine to mouse brain membranes in an assay containing 120 mM NaCl and 5 mM KCl was similar in regional distribution and pharmacological specificity to that reported previously in rat and human brain. However, the absence of ions decreased the density of the specific binding of [3H]imipramine and did not affect the equilibrium dissociation constant. Sodium was the only cation, and halides were the only anions tested that enhanced the specific binding of [3H]imipramine. Chloride did not increase the density of binding in the absence of sodium. The ion-sensitive binding of [3H]imipramine was regionally dependent and was highly correlated with the uptake of 5-hydroxytryptamine (5-HT, serotonin) into synaptosomes from brain regions. 5-HT did not inhibit the binding of [3H]imipramine in the absence of ions. Antidepressants inhibited binding in the absence and presence of ions, but in the presence of ions inhibition curves were shifted to the left and the apparent complexity of inhibition was increased. Quantitative analysis of the inhibition of [3H]imipramine binding by antidepressants conducted in the presence of ions was consistent with two binding sites. Lesion of the serotonergic input to the cerebral cortex by 5,7-dihydroxytryptamine suggested that both the 5-HT-sensitive and ion-sensitive binding of [3H]imipramine were associated with serotonergic nerve terminals. [3H]Imipramine binding displaced by desipramine, but insensitive to 5-HT and ions, was not affected by the lesion. Thus, the binding of [3H]imipramine that is displaced by desipramine, the most common assay for [3H]imipramine binding, includes a component that is not associated with brain serotonergic nerve terminals and 5-HT uptake, and, in addition, a separable component that is highly correlated with serotonergic function. These data have important implications for studies of serotonergic neurons and for the interpretation of imipramine binding data.

摘要

在含有120 mM氯化钠和5 mM氯化钾的测定中,[3H]丙咪嗪与小鼠脑膜的特异性结合在区域分布和药理学特异性上与先前在大鼠和人类大脑中报道的相似。然而,离子的缺失降低了[3H]丙咪嗪特异性结合的密度,且不影响平衡解离常数。钠是唯一能增强[3H]丙咪嗪特异性结合的阳离子,卤化物是唯一测试过的能增强其特异性结合的阴离子。在没有钠的情况下,氯离子不会增加结合密度。[3H]丙咪嗪的离子敏感结合具有区域依赖性,并且与5-羟色胺(5-HT,血清素)从脑区摄取到突触体中高度相关。在没有离子的情况下,5-HT不会抑制[3H]丙咪嗪的结合。抗抑郁药在有离子和无离子的情况下均抑制结合,但在有离子的情况下,抑制曲线向左移动,抑制的表观复杂性增加。在有离子存在的情况下,对[3H]丙咪嗪结合被抗抑郁药抑制的定量分析与两个结合位点一致。5,7-二羟基色胺对大脑皮层血清素能输入的损伤表明,[3H]丙咪嗪的5-HT敏感和离子敏感结合均与血清素能神经末梢相关。被去甲丙咪嗪取代但对5-HT和离子不敏感的[3H]丙咪嗪结合不受损伤影响。因此,被去甲丙咪嗪取代的[3H]丙咪嗪结合([3H]丙咪嗪结合的最常见测定方法)包括一个与脑血清素能神经末梢和5-HT摄取无关的成分,此外,还有一个与血清素能功能高度相关的可分离成分。这些数据对血清素能神经元的研究以及丙咪嗪结合数据的解释具有重要意义。

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