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鸽红细胞膜物理状态对腺苷酸环化酶活性的调节。1. 药物诱导的双层流动性和腺苷酸环化酶活性的平行变化。

Modulation of adenylate cyclase activity by the physical state of pigeon erythrocyte membrane. 1. Parallel drug-induced changes in the bilayer fluidity and adenylate cyclase activity.

作者信息

Salesse R, Garnier J, Leterrier F, Daveloose D, Viret J

出版信息

Biochemistry. 1982 Mar 30;21(7):1581-6. doi: 10.1021/bi00536a018.

DOI:10.1021/bi00536a018
PMID:6282308
Abstract

The fluorescence anisotropy probe perylene and the spin-labels 5-doxylsterate and 16-doxylstearate were used to estimate the order and internal microviscosity of the pigeon erythrocyte membrane upon perturbation by cationic or neutral amphipathic drugs (chlorpromazine, methochlorpromazine, tetracaine, and octanol) and an anionic drug, octanoic acid. Both methods gave identical results. The fluidity changes were found to strictly correlate with those of adenylate cyclase activity in the presence of GTP when perturbed by the drugs [Salesse, R., & Garnier, J. (1979) Biochim. Biophys. Acta 554, 102-113]. The cationic or neutral drugs, in an intermediate range of concentration, decreased the degree of organization and the internal microviscosity of the lipids together with the activity of the adenylate cyclase. At a higher concentration they reincreased them up to or higher than their initial level before the final destruction of the membrane structure and functions. This concentration effect was time dependent with tetracaine. The quaternary amine methochlorpromazine acted as chlorpromazine only on open ghosts. On intact cells, it inhibited catecholamine receptors at higher concentration and monotonously decreased the order and microviscosity, as the anionic amphipath octanoic acid did. This is taken as evidence that the inner leaflet of the bilayer is the seat for the observed multiphasic changes of viscosity and the control of adenylate cyclase and catecholamine receptors. This could stem from either a preferential intercalation or a surface effect of the amphipaths in the inner leaflet of the membrane. Since the basal activity of adenylate cyclase was not affected in the presence of drugs, it may be inferred that the enzyme holds its activity but that its stimulation is modulated by the membrane physical state.

摘要

荧光各向异性探针苝以及自旋标记物5-脱氧硬脂酸酯和16-脱氧硬脂酸酯被用于评估阳离子或中性两亲药物(氯丙嗪、甲氯丙嗪、丁卡因和辛醇)以及阴离子药物辛酸对鸽红细胞膜的有序性和内部微粘度的影响。两种方法得出了相同的结果。当受到药物干扰时,发现流动性变化与存在GTP时腺苷酸环化酶活性的变化严格相关[萨莱斯,R.,& 加尼尔,J.(1979年)《生物化学与生物物理学报》554,102 - 113]。阳离子或中性药物在中等浓度范围内,会降低脂质的有序程度和内部微粘度,同时降低腺苷酸环化酶的活性。在较高浓度时,它们会使其再次升高至或高于其初始水平,直至膜结构和功能最终被破坏。丁卡因的这种浓度效应是时间依赖性的。季胺甲氯丙嗪仅对开放的血影起作用,作用方式与氯丙嗪相同。在完整细胞上,它在较高浓度时抑制儿茶酚胺受体,并单调降低有序性和微粘度,就像阴离子两亲物辛酸一样。这被视为双层膜内小叶是观察到的粘度多相变化以及腺苷酸环化酶和儿茶酚胺受体控制的所在位置的证据。这可能源于两亲物在膜内小叶中的优先插入或表面效应。由于在药物存在下腺苷酸环化酶的基础活性未受影响,可以推断该酶保持其活性,但其刺激作用受到膜物理状态的调节。

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Modulation of adenylate cyclase activity by the physical state of pigeon erythrocyte membrane. 1. Parallel drug-induced changes in the bilayer fluidity and adenylate cyclase activity.鸽红细胞膜物理状态对腺苷酸环化酶活性的调节。1. 药物诱导的双层流动性和腺苷酸环化酶活性的平行变化。
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2
Modulation of adenylate cyclase activity by the physical state of pigeon erythrocyte membrane. 2. Fluidity-controlled coupling between the subunits of the adenylate cyclase system.鸽红细胞膜物理状态对腺苷酸环化酶活性的调节。2. 腺苷酸环化酶系统亚基之间的流动性控制偶联。
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