C6胶质瘤细胞中β 1-和β 2-和能受体的选择性脱敏。儿茶酚胺反应性的影响。

Receptor Pub Date : 1995-01-01
S W Guerrero, H Zhong, K P Minneman
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引用次数: 0

摘要

我们研究了改变β 1和β 2肾上腺素能受体(AR)亚型比例和密度对大鼠C6胶质瘤细胞环AMP (cAMP)对去甲肾上腺素(NE)和肾上腺素(EPI)反应的影响。地塞米松(DEX)增加β 2-并降低β 1-AR表达,但不改变β - ar总密度,而选择性激动剂预处理特异性下调每种亚型。这些处理组合产生的细胞具有六种不同的β 2/ β 1比率,范围从0 (100% β 1)到2.85。我们比较了NE和EPI在每种情况下对cAMP积累的影响,并观察到在大多数情况下β 1的药理学优势(NE > EPI)。然而,当β 2-AR密度超过β 1- ar的数量时,我们观察到逐渐向β 2-like药理学转变(EPI > NE),没有出现双相浓度-反应曲线。β 2/ β 1密度与NE和EPI的效价之比在促进cAMP形成方面呈显著相关(p < 0.006)。我们得出结论,在天然C6细胞中,β 1- ar似乎比β 2- ar更有效地与cAMP积累结合,但当β 2- ar的比例增加时,这两种亚型都以非加性的方式促进儿茶酚胺反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Selective desensitization of beta 1- and beta 2-andrenergic receptors in C6 glioma cells. Effects on catecholamine responsiveness.

We studied the effects of changing beta 1- and beta 2-adrenergic receptor (AR) subtype ratios and densities on cyclic AMP (cAMP) responses to norepinephrine (NE) and epinephrine (EPI) in rat C6 glioma cells. Dexamethasone (DEX) increased beta 2- and decreased beta 1-AR expression without changing total beta-AR density, whereas pretreatment with selective agonists specifically downregulated each subtype. Combinations of these treatments produced cells with six different beta 2/beta 1 ratios that ranged from 0 (100% beta 1) to 2.85. We compared the effects of NE and EPI on cAMP accumulation in each condition and observed a predominantly beta 1 pharmacology (NE > EPI) under most conditions. However, as the beta 2-AR density exceeded the number of beta 1-ARs we observed a progressive shift toward a more beta 2-like pharmacology (EPI > NE), without the appearance of biphasic concentration-response curves. The ratio of beta 2/beta 1 density correlated significantly (p < 0.006) with the ratio of the potencies of NE and EPI in increasing cAMP formation. We conclude that in native C6 cells beta 1-ARs appear to couple more efficiently to cAMP accumulation than do beta 2-ARs, but both subtypes contribute to catecholamine responses in a nonadditive manner when the proportion of beta 2-ARs is increased.

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