首页> 外文期刊>Neuropharmacology >Gene targeting demonstrates that alpha4 nicotinic acetylcholine receptor subunits contribute to expression of diverse ((3)H)epibatidine binding sites and components of biphasic (86)Rb(+) efflux with high and low sensitivity to stimulation by acetylch

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Gene targeting demonstrates that alpha4 nicotinic acetylcholine receptor subunits contribute to expression of diverse ((3)H)epibatidine binding sites and components of biphasic (86)Rb(+) efflux with high and low sensitivity to stimulation by acetylch

机译：基因靶向表明，α4烟碱乙酰胆碱受体亚基有助于表达不同的（（3）H）epibatidine结合位点和双相（86）Rb（+）外排的成分，对乙酰胆碱刺激具有高敏感性和低敏感性

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[(3)H]Epibatidine binds to nAChR subtypes in mouse brain with higher (K(D) approximately 0.02nM) and lower affinity (K(D) approximately 7nM), which can be further subdivided through inhibition by selected agonists and antagonists. These subsets are differentially affected by targeted deletion of alpha7, beta2 or beta4 subunits. Most, but not all, higher and lower affinity binding sites require beta2 (Marks, M.J., Whiteaker, P., Collins, A.C., 2006. Deletion of the alpha7, beta2 or beta4 nicotinic receptor subunit genes identifies highly expressed subtypes with relatively low affinity for [(3)H]epibatidine. Mol. Pharmacol. 70, 947-959). Effects of functional alpha4 gene deletion are reported here. Deletion of alpha4 virtually eliminated cytisine-sensitive, higher-affinity [(3)H]epibatidine binding as did beta2 deletion, confirming that these sites are alpha4beta2*-nAChR. Cytisine-resistant, higher-affinity [(3)H]epibatidine binding sites are diverse and some of these sites require alpha4 expression. Lower affinity [(3)H]epibatidine binding sites are also heterogeneous and can be subdivided into alpha-bungarotoxin-sensitive and -resistant components. Deleting alpha4 did not affect the alpha-bungarotoxin-sensitive component, but markedly reduced the alpha-bungarotoxin-resistant component. This effect was similar, but not quite identical, to the effect of beta2 deletion. This provides the first evidence that lower-affinity epibatidine binding sites in the brain require expression of alpha4 subunits. The effects of alpha4 gene targeting on receptor function were measured using a (86)Rb(+) efflux assay. Concentration-effect curves for ACh-stimulated (86)Rb(+) efflux are biphasic (EC(50) values=3.3muM and 300muM). Targeting alpha4 produced substantial gene-dose dependent reductions in both phases in whole brain and in most of the 14 brain regions assayed. These effects are very similar to those following deletion of beta2. Thus, alpha4beta2*-nAChRs mediate a significant fraction of both phases of ACh stimulated (86)Rb(+) efflux.

机译：[（3）H] Epibatidine以较高的（K（D）约0.02nM）和较低的亲和力（K（D）约7nM）结合到小鼠脑中的nAChR亚型，可以通过选择的激动剂和拮抗剂抑制而进一步细分。这些子集受到有针对性的alpha7，beta2或beta4亚基缺失的影响。大多数但不是全部，较高和较低的亲和力结合位点都需要beta2（Marks，MJ，Whiteaker，P.，Collins，AC，2006。删除alpha7，beta2或beta4烟碱样受体亚基基因可确定亲和力较低的高表达亚型[（3）H]表巴替丁的分子量（Mol.Pharmacol.70，947-959）。这里报道了功能性α4基因缺失的影响。删除alpha4几乎消除了对胱氨酸敏感的，更高亲和力的[（3）H]依帕替丁结合，与beta2删除一样，确认这些位点是alpha4beta2 * -nAChR。胞嘧啶抗性，较高亲和力的[（3）H] epibatidine结合位点是多样的，其中一些位点需要alpha4表达。较低亲和力的[（3）H]表巴替丁结合位点也是异质的，可以细分为对α-邦加罗毒素的敏感和耐药的组件。删除α4不会影响对α-真菌毒素敏感的组件，但会显着降低对α-真菌毒素抗性的组件。此效果与beta2删除的效果相似但不完全相同。这提供了第一个证据，即大脑中较低亲和力的Epibatidine结合位点需要表达alpha4亚基。使用（86）Rb（+）外排试验测量了针对受体功能的alpha4基因的作用。 ACh刺激的（86）Rb（+）外排的浓度效应曲线是双相的（EC（50）值=3.3μM和300μM）。靶向α4在整个大脑和所检测的14个大脑区域的大多数阶段的两个阶段均产生了显着的基因剂量依赖性降低。这些效果与删除beta2之后的效果非常相似。因此，alpha4beta2 * -nAChRs介导ACh刺激的（86）Rb（+）外排的两个阶段的很大一部分。

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《Neuropharmacology》 |2007年第3期|共16页
作者
Marks MJ; Meinerz NM; Drago J; Collins AC;
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正文语种 eng
中图分类药理学;
关键词
epibatidine; beta2; Binding Sites; 结合部位;

机译：epibatidine;beta2;Binding Sites;结合部位;

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1. Gene targeting demonstrates that alpha4 nicotinic acetylcholine receptor subunits contribute to expression of diverse ((3)H)epibatidine binding sites and components of biphasic (86)Rb(+) efflux with high and low sensitivity to stimulation by acetylch [J] . Marks MJ, Meinerz NM, Drago J, Neuropharmacology . 2007,第3期

机译：基因靶向表明，α4烟碱乙酰胆碱受体亚基有助于表达不同的（（3）H）epibatidine结合位点和双相（86）Rb（+）外排的成分，对乙酰胆碱刺激具有高敏感性和低敏感性
2. Subsets of acetylcholine-stimulated 86Rb+ efflux and (125I)-epibatidine binding sites in C57BL/6 mouse brain are differentially affected by chronic nicotine treatment. [J] . Marks MJ, Rowell PP, Cao JZ, Neuropharmacology . 2004,第8期

机译：C57BL / 6小鼠大脑中乙酰胆碱刺激的86Rb +外排和（125I）-依巴替丁结合位点的亚集受到慢性尼古丁治疗的差异影响。
3. 86Rb+ efflux mediated by alpha4beta2*-nicotinic acetylcholine receptors with high and low-sensitivity to stimulation by acetylcholine display similar agonist-induced desensitization. [J] . Marks MJ, Meinerz NM, Brown RW, Biochemical Pharmacology . 2010,第8期

机译：由α4beta2*烟碱型乙酰胆碱受体介导的86Rb +外排对乙酰胆碱刺激具有高敏感性和低敏感性，表现出相似的激动剂诱导的脱敏作用。
4. Gene Targeting Demonstrates That α4 Nicotinic Acetylcholine Receptor Subunits Contribute to Expression of Diverse 3HEpibatidine Binding Sites and Components of Biphasic 86Rb+ Efflux With High and Low Sensitivity to Stimulation by Acetylcholine [O] . Michael J. Marks, Natalie M. Meinerz, John Drago, -1

机译：基因靶向证明α4烟碱乙酰胆碱受体亚基有助于表达不同的3H Epibatidine结合位点和双相86Rb +外排组分对乙酰胆碱刺激具有高和低敏感性。
5. 86Rb+ efflux mediated by α4β2*-nicotinic acetylcholine receptors with high and low-sensitivity to stimulation by acetylcholine display similar agonist-induced desensitization [O] . Michael J. Marks, Natalie M. Meinerz, Robert W.B. Brown, 2010

机译：由乙酰胆碱显示相似的激动剂诱导的脱敏，由α4β2* - 高致乙酰胆碱受体介导的α4β2* - 硝基乙酰胆碱受体介导的α4β2* - 肌约乙酰胆碱受体介导。

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