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Mechanisms for the emergence of catecholamine‐sensitive adenylate cyclase and β‐adrenergic receptors in cultured hepatocytes
[摘要]

Adult male rat hepatocytes, which normally respond poorly to β-adrenergic agents, acquire such responsiveness during primary monolayer culture. We here show that the rise in catecholamine-sensitive adenylate cyclase activity in hepatocytes in vitro is closely paralleled by an increase in the ability to bind the β-adrenoceptor ligand [125I]cyanopindolol. The emergence of β-adrenergic responsiveness did not require cell attachment or serum. Addition of dexamethasone, insulin, thyroxine or dihydortestosterone to the cultures, singly or in combination, did not prevent the augmented β-adrenergic responsiveness. The increase in catecholamine-sensitive adenylate cyclase activity and [125I]cyanopindolol binding could be blocked by cycloheximide or actinomycin D. Exposure of the cultures to isoproterenol at 3-hourly intervals led to a dose-dependent suppression of the rise in isoproterenol-responsive adenylate cyclase and prevented the increase in β-adrenoceptor binding.

[发布日期]  [发布机构] 
[效力级别]  [学科分类] 生物化学/生物物理
[关键词] β-Adrenergic receptor;Adenylate cyclase;Actinomycin D;Cycloheximide;Rat hepatocyte;Primary culture;MIX;methylisobutylxanthine;ICYP;iodocyanopindolol;CHX;cycloheximide;Act. D;actinomycin D [时效性] 
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