转染的人腺苷A1受体与CHO-K1细胞中组成型P2嘌呤受体的肌醇磷酸反应之间的协同作用。
Synergy between the inositol phosphate responses to transfected human adenosine A1-receptors and constitutive P2-purinoceptors in CHO-K1 cells.
作者信息
Megson A C, Dickenson J M, Townsend-Nicholson A, Hill S J
机构信息
Department of Physiology & Pharmacology, Medical School, Queen's Medical Centre, Nottingham.
出版信息
Br J Pharmacol. 1995 Aug;115(8):1415-24. doi: 10.1111/j.1476-5381.1995.tb16632.x.
Abstract
- The effect of adenosine A1-receptor and P2-purinoceptor agonists on [3H]-inositol phosphate accumulation has been investigated in CHO-K1 cells transfected with the human adenosine A1-receptor. 2. Adenosine receptor agonists stimulated [3H]-inositol phosphate accumulation in CHO-K1 cells with a rank potency order of N6-cyclopentyladenosine (CPA) > 5'-N-ethylcarboxamidoadenosine (NECA) > 2-chloroadenosine > N6-2-(4-aminophenyl) ethyladenosine (APNEA). The responses to both CPA and APNEA were antagonized by the A1 selective antagonist, 1,3-dipropylcyclopentylxanthine (DPCPX) yielding KD values of 1.2 nM and 4.3 nM respectively. 3. ATP, UTP and ATP gamma S were also able to stimulate [3H]-inositol phosphate accumulation in these cells with EC50 values of 1.9 microM, 1.3 microM and 5.0 microM respectively. 2-Methyl-thio-ATP was a weak agonist of this response (EC50 > 100 microM). 4. The [3H]-inositol phosphate response to CPA was completely attenuated by pertussis toxin treatment (24 h; 100 ng ml-1). In contrast, the responses to ATP, UTP and ATP gamma S were only reduced by circa 30% in pertussis toxin-treated cells. 5. The simultaneous addition of CPA and either ATP, UTP or ATP gamma S produced a large augmentation of [3H]-inositol phospholipid hydrolysis. This was due to an increase in the maximal response and was significantly greater than the predicted additive response for activation of these two receptor systems. The synergy was not observed in pertussis toxin-treated cells. 6. No synergy was observed between the [3H]-inositol phosphate responses to histamine and ATP in CHO-K1 cells transfected with the bovine histamine H1-receptor. In these cells the response to histamine was completely resistant to inhibition by pertussis toxin treatment. 7. This study provides a clear demonstration of a synergy between pertussis toxin-sensitive and insensitive receptor systems in a model cell system which is an ideal host for transfected cDNA sequences. This model system should provide a unique opportunity to unravel the mechanisms underlying this example of receptor cross-talk involving phospholipase C.
摘要
- 已在转染了人腺苷A1受体的CHO-K1细胞中研究了腺苷A1受体和P2嘌呤受体激动剂对[3H] - 肌醇磷酸积累的影响。2. 腺苷受体激动剂刺激CHO-K1细胞中[3H] - 肌醇磷酸积累,其效价顺序为N6-环戊基腺苷(CPA)> 5'-N-乙基羧酰胺腺苷(NECA)> 2-氯腺苷> N6-2-(4-氨基苯基)乙基腺苷(APNEA)。A1选择性拮抗剂1,3-二丙基环戊基黄嘌呤(DPCPX)拮抗了对CPA和APNEA的反应,KD值分别为1.2 nM和4.3 nM。3. ATP、UTP和ATPγS也能够刺激这些细胞中[3H] - 肌醇磷酸积累,EC50值分别为1.9 microM、1.3 microM和5.0 microM。2-甲基硫代-ATP是该反应的弱激动剂(EC50> 100 microM)。4. 百日咳毒素处理(24小时;100 ng/ml)可完全减弱对CPA的[3H] - 肌醇磷酸反应。相比之下,在百日咳毒素处理的细胞中,对ATP、UTP和ATPγS的反应仅降低约30%。5. 同时添加CPA和ATP、UTP或ATPγS可使[3H] - 肌醇磷脂水解大幅增加。这是由于最大反应增加,且明显大于激活这两个受体系统的预测相加反应。在百日咳毒素处理的细胞中未观察到协同作用。6. 在转染了牛组胺H1受体的CHO-K1细胞中,对组胺和ATP的[3H] - 肌醇磷酸反应之间未观察到协同作用。在这些细胞中,对组胺的反应完全抵抗百日咳毒素处理的抑制。7. 本研究清楚地证明了在一个模型细胞系统中,百日咳毒素敏感和不敏感受体系统之间存在协同作用,该模型细胞系统是转染cDNA序列的理想宿主。这个模型系统应该提供一个独特的机会来揭示这种涉及磷脂酶C的受体相互作用实例背后的机制。
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