环磷酸腺苷升高剂对犬培养气管平滑肌细胞中缓激肽和卡巴胆碱诱导的信号转导的影响。

The effect of cyclic AMP elevating agents on bradykinin- and carbachol-induced signal transduction in canine cultured tracheal smooth muscle cells.

作者信息

Yang C M, Hsia H C, Luo S F, Hsieh J T, Ong R

机构信息

Department of Pharmacology, Chang Gung Medical College, Kwei-San, Tao-Yuan, Taiwan.

出版信息

Br J Pharmacol. 1994 Jul;112(3):781-8. doi: 10.1111/j.1476-5381.1994.tb13147.x.

DOI:10.1111/j.1476-5381.1994.tb13147.x

PMID:7921603

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1910198/

Abstract

The effects of cholera toxin (CTX), forskolin and dibutyryl cyclic AMP on bradykinin (BK)- and carbachol-induced accumulation of inositol phosphates (IPs) and Ca2+ mobilization were investigated in canine cultured tracheal smooth muscle cells (TSMCs). The BK-induced responses were mediated via a G protein which was not inhibited by CTX or pertussis toxin treatment. 2. BK-stimulated IPs accumulation and Ca2+ mobilization were potentiated by CTX (10 micrograms ml-1) pretreatment which was time-dependent. Maximal increase of these responses occurred after 24 h treatment with CTX. The concentration-effect relationship of BK-induced responses were shifted to the left and BK was substantially more effective in CTX-treated cells than in the control cells. This enhancing effect of CTX did not occur with carbachol. 3. Short-term (< 4 h) treatment with forskolin (10 microM) or dibutyryl cyclic AMP (1 mM) failed to accentuate BK-induced responses, but long-term (> 4 h) treatment of TSMCs with these agents mimicked the enhancing effect of CTX, suggesting that CTX-induced enhancement of BK responsiveness might be due to a rise in cyclic AMP. 4. Prolonged treatment of TSMCs with these agents was accompanied by an increase in cell surface [3H]-BK binding sites, which was inhibited by concurrent incubation with cycloheximide, an inhibitor of protein biosynthesis. Cycloheximide also abolished the potentiating actions of CTX, forskolin, and dibutyryl cyclic AMP on BK-induced IPs formation and Ca2+ mobilization. 5. The locus of this enhancement was further investigated by examining the effects of CTX, forskolin and dibutyryl cyclic AMP on A1F4(-)-induced IPs accumulation in canine TSMCs. AIF4-induced IPs accumulation was not affected by CTX, forskolin, or dibutyryl cyclic AMP treatment, supporting the contention that this stimulatory effect is located at the BK receptor level.6. These results demonstrate that the augmentation of BK-induced IPs accumulation and Ca2+mobilization produced by CTX, forskolin and dibutyryl cyclic AMP involves a cyclic AMP-dependent mechanism which is induced by a sustained increase in the level of intracellular cyclic AMP. CTX and forskolin may promote an increase of the synthesis of BK receptors, and thereby enhance BK-induced responses.

摘要

在犬类培养的气管平滑肌细胞（TSMCs）中，研究了霍乱毒素（CTX）、福斯高林和二丁酰环磷腺苷对缓激肽（BK）和卡巴胆碱诱导的肌醇磷酸（IPs）积累及钙离子动员的影响。BK诱导的反应是通过一种G蛋白介导的，该G蛋白不受CTX或百日咳毒素处理的抑制。2. CTX（10微克/毫升）预处理可增强BK刺激的IPs积累和钙离子动员，且具有时间依赖性。用CTX处理24小时后，这些反应出现最大程度的增加。BK诱导反应的浓度-效应关系向左移动，并且在CTX处理的细胞中BK比对照细胞更有效。卡巴胆碱未出现CTX的这种增强作用。3. 用福斯高林（10微摩尔）或二丁酰环磷腺苷（1毫摩尔）进行短期（<4小时）处理未能增强BK诱导的反应，但用这些试剂对TSMCs进行长期（>4小时）处理可模拟CTX的增强作用，表明CTX诱导的BK反应性增强可能是由于环磷腺苷水平升高所致。4. 用这些试剂对TSMCs进行长时间处理会伴随着细胞表面[3H]-BK结合位点的增加，同时与蛋白质生物合成抑制剂环己酰亚胺一起孵育可抑制这种增加。环己酰亚胺还消除了CTX、福斯高林和二丁酰环磷腺苷对BK诱导的IPs形成和钙离子动员的增强作用。5. 通过检查CTX、福斯高林和二丁酰环磷腺苷对犬类TSMCs中A1F4(-)诱导的IPs积累的影响，进一步研究了这种增强作用的位点。AIF4诱导的IPs积累不受CTX、福斯高林或二丁酰环磷腺苷处理的影响，支持了这种刺激作用位于BK受体水平的观点。6. 这些结果表明，CTX、福斯高林和二丁酰环磷腺苷引起的BK诱导的IPs积累和钙离子动员的增强涉及一种环磷腺苷依赖性机制，该机制是由细胞内环磷腺苷水平的持续升高诱导的。CTX和福斯高林可能促进BK受体合成的增加，从而增强BK诱导的反应。