HEL 92.1.7细胞中G(i/o)介导的α(2A)-肾上腺素能受体反应的激动剂转运
Agonist trafficking of G(i/o)-mediated alpha(2A)-adrenoceptor responses in HEL 92.1.7 cells.
作者信息
Kukkonen J P, Jansson C C, Akerman K E
机构信息
Department of Physiology, Division of Cell Physiology, Uppsala University, BMC, P.O. Box 572, S-75123 Uppsala, Sweden.
出版信息
Br J Pharmacol. 2001 Apr;132(7):1477-84. doi: 10.1038/sj.bjp.0703964.
Abstract
- The ability of 19 agonists to elevate Ca(2+) and inhibit forskolin-induced cyclic AMP elevation through alpha(2A)-adrenoceptors in HEL 92.1.7 cells was investigated. Ligands of catecholamine-like- (five), imidazoline- (nine) and non-catecholamine-non-imidazoline-type (five) were included. 2. The relative maximum responses were similar in both assays. Five ligands were full or nearly full agonists, six produced 20 - 70% of the response to a full agonist and the remaining eight gave lower responses (< 20%) so that their potencies were difficult to evaluate. 3. Marked differences in the potencies of the agonists with respect to the two measured responses were seen. The catecholamines were several times less potent in decreasing cyclic AMP than in increasing Ca(2+), whereas the other, both imidazoline and ox-/thiazoloazepine ligands, were several times more potent with respect to the former than the latter response. For instance, UK14,304 was more potent than adrenaline with respect to the cyclic AMP response but less potent than adrenaline with respect to the Ca(2+) response. 4. All the responses were sensitive to pertussis toxin-pretreatment. Also the possible role of PLA(2), beta-adrenoceptors or ligand transport or metabolism as a source of error could be excluded. The results suggest that the active receptor states produced by catecholamines and the other agonists are markedly different and therefore have different abilities to activate different signalling pathways.
摘要
- 研究了19种激动剂通过HEL 92.1.7细胞中的α(2A)-肾上腺素能受体升高Ca(2+)并抑制福斯可林诱导的环磷酸腺苷升高的能力。其中包括儿茶酚胺样(5种)、咪唑啉(9种)和非儿茶酚胺-非咪唑啉型(5种)配体。2. 两种测定方法中的相对最大反应相似。5种配体为完全或几乎完全激动剂,6种产生的反应为完全激动剂反应的20%-70%,其余8种反应较低(<20%),因此难以评估其效力。3. 观察到激动剂在两种测量反应的效力上存在显著差异。儿茶酚胺在降低环磷酸腺苷方面的效力比升高Ca(2+)时低几倍,而其他配体,包括咪唑啉和氧/噻唑并氮杂卓配体,在前一种反应中的效力比后一种反应高几倍。例如,UK14,304在环磷酸腺苷反应方面比肾上腺素更有效,但在Ca(2+)反应方面比肾上腺素效力低。4. 所有反应对百日咳毒素预处理敏感。也可以排除磷脂酶A(2)、β-肾上腺素能受体或配体转运或代谢作为误差来源的可能作用。结果表明,儿茶酚胺和其他激动剂产生的活性受体状态明显不同,因此激活不同信号通路的能力也不同。
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3
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4
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