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慢性激动剂输注对脑烟碱受体的调节作用。

Regulation of brain nicotinic receptors by chronic agonist infusion.

作者信息

Bhat R V, Turner S L, Selvaag S R, Marks M J, Collins A C

机构信息

School of Pharmacy, University of Colorado, Boulder 80309.

出版信息

J Neurochem. 1991 Jun;56(6):1932-9. doi: 10.1111/j.1471-4159.1991.tb03450.x.

Abstract

Several studies have demonstrated that chronic treatment with nicotine elicits an increase in the number of brain nicotinic receptors. To determine whether this effect is elicited by other nicotinic agonists found in tobacco, the effects of chronic infusion with nicotine on brain nicotinic receptors were compared with those after anabasine and lobeline. C57BL/6 mice were infused with saline or equimolar doses (18.5 mumol/kg/h) of nicotine, anabasine, or lobeline for 8 days. Nicotinic receptors, quantified by the binding of [3H]nicotine and [125I]iodo-alpha-bungarotoxin (alpha-[125I]BTX), and muscarinic receptors, quantified by the binding of [3H]quinuclidinyl benzilate ([3H]QNB), were then assayed in eight brain regions. An increase in [3H]nicotine binding was observed in all regions except cerebellum following chronic infusion with nicotine and anabasine, whereas lobeline did not alter the number or affinity of these binding sites. This increase was due to changes in Bmax and not in the affinity of the receptor for the ligand (KD). A slight increase in alpha-[125I]BTX binding was observed in cortex following chronic anabasine infusion. [3H]QNB binding sites were largely unaltered following chronic infusion with any of the nicotinic analogs. The levels of the agonists in the brain were also determined after chronic treatment, and the amounts of lobeline and anabasine were found to be higher than that of nicotine. Thus, the failure of lobeline to elicit changes in nicotine binding is not due to reduced brain concentrations.

摘要

多项研究表明,长期使用尼古丁进行治疗会使脑烟碱受体数量增加。为了确定这种效应是否由烟草中发现的其他烟碱激动剂引起,将尼古丁长期输注对脑烟碱受体的影响与新烟草碱和洛贝林的影响进行了比较。给C57BL/6小鼠输注生理盐水或等摩尔剂量(18.5 μmol/kg/h)的尼古丁、新烟草碱或洛贝林,持续8天。然后在八个脑区检测通过[3H]尼古丁和[125I]碘化α-银环蛇毒素(α-[125I]BTX)结合定量的烟碱受体,以及通过[3H]喹核醇基苯甲酸酯([3H]QNB)结合定量的毒蕈碱受体。长期输注尼古丁和新烟草碱后,除小脑外的所有区域均观察到[3H]尼古丁结合增加,而洛贝林并未改变这些结合位点的数量或亲和力。这种增加是由于Bmax的变化,而非受体对配体的亲和力(KD)的变化。长期输注新烟草碱后,在皮层观察到α-[125I]BTX结合略有增加。长期输注任何一种烟碱类似物后,[3H]QNB结合位点基本未改变。长期治疗后还测定了脑内激动剂的水平,发现洛贝林和新烟草碱的含量高于尼古丁。因此,洛贝林未能引起尼古丁结合变化并非由于脑内浓度降低。

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