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外文期刊>The biochemical journal
>Cholera toxin impairment of opioid-mediated inhibition of adenylate cyclase in neuroblastoma × glioma hybrid cells is due to a toxin-induced decrease in opioid receptor levels
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Cholera toxin impairment of opioid-mediated inhibition of adenylate cyclase in neuroblastoma × glioma hybrid cells is due to a toxin-induced decrease in opioid receptor levels
pCholera toxin treatment (up to 1 microgram/ml, 16 h) of neuroblastoma x glioma hybrid NG108-15 cells produced a decrease of some 35% in both delta opioid receptor-mediated stimulation of high-affinity GTPase activity and inhibition of forskolin-amplified adenylate cyclase. Coincident with these decreases was a down-regulation of some 35% in the delta opioid receptor population. A similar pattern of a decrease in signalling capacity was noted for the alpha 2B-adrenergic receptor in these cells after cholera toxin treatment. Half-maximal effects of cholera toxin on all of the parameters assayed were noted at concentrations between 2 and 5 ng/ml. Neither levels of Gi2, as assessed by immunoblotting with specific antisera, nor the intrinsic activity of the alpha subunit of the guanine-nucleotide-binding protein which acts as the inhibitory G-protein of the adenylate cyclase in these cells, as assessed by guanosine 5′-[beta gamma-imido]triphosphate (Gpp[NH]p)-mediated inhibition of adenylate cyclase, was lowered by cholera toxin treatment. Furthermore, levels of another pertussis toxin-sensitive G-protein (Go) expressed by these cells was also not lowered by cholera toxin treatment. However, as previously noted in other cells [Milligan, Unson & Wakelam (1989) Biochem. J. 262, 643-649], marked down-regulation of the alpha subunit of the stimulatory G-protein (Gs) of the adenylate cyclase cascade was observed in response to cholera toxin treatment. Previous studies [Klee, Milligan, Simonds & Tocque (1985) Mol. Aspects Cell Regul. 4, 117-129] have shown that cholera toxin treatment can result in a decrease in the maximal effectiveness of agonists which function to inhibit adenylate cyclase. These data have been used as evidence to suggest a functional interaction between Gs and ‘Gi’. The results provided herein demonstrate that such effects of the toxin can be explained adequately by a decrease in the number of receptors that function to produce inhibition of adenylate cyclase./p
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机译:p对神经母细胞瘤×胶质瘤杂交NG108-15细胞的霍乱毒素处理(高达1微克/毫升,16小时)使δ阿片受体介导的对高亲和力GTPase活性的刺激和对AGF的抑制作用均降低了约35%。福司可林扩增的腺苷酸环化酶。与这些减少同时出现的是阿片类阿片受体群体中约35%的下调。在霍乱毒素处理后,这些细胞中的α2B-肾上腺素受体的信号传导能力下降的模式类似。在2到5 ng / ml的浓度下,霍乱毒素对所有测定参数的半数最大效应被注意到。通过鸟嘌呤5评估,既不通过特异性抗血清免疫印迹评估的Gi2含量水平,也不作为这些细胞中腺苷酸环化酶抑制性G蛋白的鸟嘌呤核苷酸结合蛋白的α亚基的内在活性。霍乱毒素治疗降低了'-β-γ-亚氨基三磷酸(Gpp [NH] p)介导的腺苷酸环化酶抑制作用。此外,霍乱毒素处理也不会降低这些细胞表达的另一种百日咳毒素敏感的G蛋白(Go)的水平。然而,如先前在其他单元中所指出的[Milligan,Unson& A. Wakelam(1989)生物化学。 J. 262,643-649],观察到响应霍乱毒素治疗,腺苷酸环化酶级联的刺激性G蛋白(Gs)的α亚基明显下调。以前的研究[Klee,Milligan,Simonds&托克(1985)方面细胞法规。 [4,117-129]显示霍乱毒素治疗可导致起抑制腺苷酸环化酶作用的激动剂的最大功效降低。这些数据已被用作暗示Gs和“ Gi”之间功能相互作用的证据。本文提供的结果表明,可以通过减少产生抑制腺苷酸环化酶功能的受体数量来充分解释这种毒素的作用。
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