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小鼠α2C肾上腺素能受体表达的基因改变:对右美托咪定(一种非亚型选择性α2肾上腺素能受体激动剂)的运动、体温降低及神经化学效应的影响。

Genetic alteration of alpha 2C-adrenoceptor expression in mice: influence on locomotor, hypothermic, and neurochemical effects of dexmedetomidine, a subtype-nonselective alpha 2-adrenoceptor agonist.

作者信息

Sallinen J, Link R E, Haapalinna A, Viitamaa T, Kulatunga M, Sjöholm B, Macdonald E, Pelto-Huikko M, Leino T, Barsh G S, Kobilka B K, Scheinin M

机构信息

Department of Pnarmacology and Clinical Pharmacology, University of Turku, Finland.

出版信息

Mol Pharmacol. 1997 Jan;51(1):36-46. doi: 10.1124/mol.51.1.36.

Abstract

alpha 2-Adrenergic receptors (alpha 2-ARs) regulate many physiological functions and are targets for clinically important antihypertensive and anesthetic agents. Three human and mouse genes encoding alpha 2-AR subtypes (alpha 2A, alpha 2B, and alpha 2C) have been cloned. We investigated the involvement of the alpha 2C-AR in alpha 2-adrenergic pharmacology by applying molecular genetic techniques to alter the expression of alpha 2C-AR in mice. The effects of dexmedetomidine, a subtype-nonselective alpha 2-AR agonist, on monoamine turnover in brain and on locomotor activity were similar in mice with targeted inactivation of the alpha 2C-AR gene and in their controls, but the hypothermic effect of the alpha 2-AR agonist was significantly attenuated by the receptor gene inactivation. Correspondingly, another strain of transgenic mice with 3-fold overexpression of alpha 2C-AR in striatum and other brain regions expressing alpha 2C-AR showed normal reductions in brain monoamine metabolism and locomotor activity after dexmedetomidine, but their hypothermic response to the alpha 2C-AR agonists was significantly accentuated. The hypothermic effect of alpha 2-AR agonists thus seems to be mediated in part by alpha 2C-AR. Some small but statistically significant differences between the strains were also noted in brain dopamine metabolism. Lack of alpha 2C-AR expression was linked with reduced levels of homovanillic acid in brain, and mice with increased alpha 2C-AR expression had elevated concentrations of the dopamine metabolite compared with their controls.

摘要

α2-肾上腺素能受体(α2-ARs)调节多种生理功能,是临床上重要的抗高血压和麻醉药物的作用靶点。已克隆出编码α2-AR亚型(α2A、α2B和α2C)的3个人类和小鼠基因。我们通过应用分子遗传学技术改变小鼠体内α2C-AR的表达,研究了α2C-AR在α2-肾上腺素能药理学中的作用。在α2C-AR基因靶向失活的小鼠及其对照小鼠中,右美托咪定(一种亚型非选择性α2-AR激动剂)对脑内单胺周转和运动活性的影响相似,但α2-AR激动剂的体温降低作用因受体基因失活而显著减弱。相应地,另一株在纹状体和其他表达α2C-AR的脑区中α2C-AR过表达3倍的转基因小鼠,在给予右美托咪定后,脑单胺代谢和运动活性正常降低,但其对α2C-AR激动剂的体温降低反应显著增强。因此,α2-AR激动剂的体温降低作用似乎部分由α2C-AR介导。在脑多巴胺代谢方面,不同品系之间也存在一些虽小但具有统计学意义的差异。缺乏α2C-AR表达与脑内高香草酸水平降低有关,与对照小鼠相比,α2C-AR表达增加的小鼠多巴胺代谢物浓度升高。

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