赛庚啶抑制胰岛素分泌的机制。
Mechanism by which cyproheptadine inhibits insulin secretion.
作者信息
Donatsch P, Lowe D A, Richardson B P, Taylor P
出版信息
Br J Pharmacol. 1980 Nov;70(3):355-62. doi: 10.1111/j.1476-5381.1980.tb08710.x.
Abstract
1 Isolated islets of Langerhans from the rat have been used in studies designed to elucidate the mechanism by which cyproheptadine inhibits insulin secretion. 2 D-Glucose and tolbutamide, both of which require extracellular Ca2+ to produce insulin release, failed to evoke a secretory response from islets pretreated with cyproheptadine. Conversely veratridine, the calcium ionophore A23187 and theophylline, all of which are capable of mobilizing sufficient intracellular Ca2+ to evoke insulin secretion in the absence of extracellular Ca2+, produced similar responses from cyproheptadine pretreated and control islets. 3 Cyproheptadine completely inhibited Ca2+ uptake induced by D-glucose and high Ko+, two agents which depolarize the islet beta-cell membrane, whilst Ca2+ uptake elicited by removal of extracellular Na+ (i.e. Na+-Ca2+ counter transport) was only slightly reduced. 4 A significant increase in Na+ uptake produced by veratridine was sensitive to tetrodoxin but only partially reduced by cyproheptadine. 5 These results suggest that cyproheptadine inhibits depolarization-dependent calcium entry into pancreatic beta-cells.
摘要
- 大鼠分离的胰岛已被用于旨在阐明赛庚啶抑制胰岛素分泌机制的研究中。2. D-葡萄糖和甲苯磺丁脲都需要细胞外Ca2+来产生胰岛素释放,但它们未能引起经赛庚啶预处理的胰岛的分泌反应。相反,藜芦碱、钙离子载体A23187和茶碱,在没有细胞外Ca2+的情况下都能够动员足够的细胞内Ca2+来引发胰岛素分泌,它们对经赛庚啶预处理的胰岛和对照胰岛产生了相似的反应。3. 赛庚啶完全抑制了由D-葡萄糖和高K+诱导的Ca2+摄取,这两种物质会使胰岛β细胞膜去极化,而去除细胞外Na+(即Na+-Ca2+逆向转运)引起的Ca2+摄取仅略有减少。4. 藜芦碱产生的Na+摄取显著增加对河豚毒素敏感,但仅被赛庚啶部分降低。5. 这些结果表明,赛庚啶抑制依赖去极化的钙进入胰腺β细胞。
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The stimulus-secretion coupling of glucose-induced insulin release. 3. Uptake of 45 calcium by isolated islets of Langerhans.葡萄糖诱导胰岛素释放的刺激-分泌偶联。3. 分离的胰岛对45钙的摄取。
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Diabetes. 1972 Oct;21(10):987-98. doi: 10.2337/diab.21.10.987.
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Diabetologia. 1973 Jun;9(3):167-73. doi: 10.1007/BF01219778.
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The stimulus-secretion coupling of glucose-induced insulin release. VII. A proposed site of action for adenosine-3',5'-cyclic monophosphate.葡萄糖诱导胰岛素释放的刺激-分泌偶联。VII. 3',5'-环磷酸腺苷的一个拟作用位点。
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