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一种产生降钙素的人类癌细胞系中的降钙素反应性腺苷酸环化酶

Calcitonin-responsive adenylate cyclase in a calcitonin-producing human cancer cell line.

作者信息

Hunt N H, Ellison M, Underwood J C, Martin T J

出版信息

Br J Cancer. 1977 Jun;35(6):777-84. doi: 10.1038/bjc.1977.119.

Abstract

A calcitonin-responsive adenylate cyclase has been found in a cell line of a poorly differentiated bronchial carcinoma (BEN cells). The cells have previously been shown to secrete an immunoreactive form of calcitonin in culture. Salmon calcitonin (SCT), porcine calcitonin (PCT) and human calcitonin (CT-M) all stimulated adenylate cyclase activity in particulate preparations. CT-M sulphoxide had little effect. The concentrations of the calcitonins required for half the maximum activation of adenylate cyclase were 6-8, 18 and 90 nm respectively. SCT (30pm) and CT-M (60 pm) increased the intracellular concentration of cyclic AMP from 11-2+/-0-2 (s.e.) to 18-2+/-0-2 and 16-7+/-0-2 respectively over a 2-5-min period. SCT (labelled with 125I) bound to particulate preparations of Ben cells, and competition for binding occurred with unlabelled SCT and CT-M. The concentration of SCT required for half the maximum inhibition of [125I]SCT binding was 11 nm. CT-M sulphoxide inhibited only at high concentration (3 micron). The characteristics of the adenylate cyclase response to SCT did not change over the period between cell adhesion (after subculture) and confluence. However, pre-incubation of cells for 4 h with SCT (150 nm) abolished the subsequent adenylate cyclase response of particulate preparations to further hormone. The practical difficulties encountered in purifying and quantifying the large-mol.-wt. form of CT-M secreted by BEN cells has precluded direct investigation of the potential relationship between hormone secretion and the occurrence of the calcitonin receptor. This relationship is discussed in terms of its possible biological significance.

摘要

在一种低分化支气管癌的细胞系(BEN细胞)中发现了一种降钙素反应性腺苷酸环化酶。此前已证明这些细胞在培养中会分泌一种免疫反应性形式的降钙素。鲑鱼降钙素(SCT)、猪降钙素(PCT)和人降钙素(CT-M)均能刺激微粒体制剂中的腺苷酸环化酶活性。CT-M亚砜的作用很小。使腺苷酸环化酶达到最大激活一半所需的降钙素浓度分别为6 - 8、18和90 nM。在2 - 5分钟内,SCT(30 pM)和CT-M(60 pM)分别使细胞内环磷酸腺苷(cAMP)浓度从11.2±0.2(标准误)增加到18.2±0.2和16.7±0.2。125I标记的SCT与BEN细胞的微粒体制剂结合,未标记的SCT和CT-M会竞争结合。使[125I]SCT结合抑制一半所需的SCT浓度为11 nM。CT-M亚砜仅在高浓度(3 μM)时才有抑制作用。从细胞贴壁(传代培养后)到汇合期间,腺苷酸环化酶对SCT的反应特性没有变化。然而,用SCT(150 nM)对细胞进行4小时预孵育后,微粒体制剂随后对进一步激素的腺苷酸环化酶反应消失。纯化和定量BEN细胞分泌的大分子量形式的CT-M时遇到的实际困难阻碍了对激素分泌与降钙素受体出现之间潜在关系的直接研究。本文从其可能的生物学意义方面对这种关系进行了讨论。

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Calcitonin and calcitonin receptors: bone and beyond.降钙素与降钙素受体:骨骼及其他方面
Int J Exp Pathol. 2000 Dec;81(6):405-22. doi: 10.1046/j.1365-2613.2000.00176.x.

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Human calcitonin.人降钙素。
Nature. 1968 Dec 7;220(5171):984-6. doi: 10.1038/220984a0.
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A highly sensitive adenylate cyclase assay.一种高灵敏度的腺苷酸环化酶检测方法。
Anal Biochem. 1974 Apr;58(2):541-8. doi: 10.1016/0003-2697(74)90222-x.
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Ectopic hormone production by non-endocrine tumours.非内分泌肿瘤产生异位激素。
Clin Endocrinol (Oxf). 1974 Jul;3(3):263-99. doi: 10.1111/j.1365-2265.1974.tb01801.x.

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