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胎鼠β细胞中葡萄糖诱导的胰岛素释放现象

Appearance of glucose-induced insulin release in fetal rat beta-cells.

作者信息

Bergsten P, Aoyagi K, Persson E, Eriksson U J, Hellerström C

机构信息

Department of Medical Cell Biology, Uppsala University, Sweden.

出版信息

J Endocrinol. 1998 Jul;158(1):115-20. doi: 10.1677/joe.0.1580115.

Abstract

Fetal rat pancreatic cells were isolated from pancreatic primordia on days 12-14 of pregnancy and cultured for 48 h in the presence of 5 mmol/l glucose. Insulin accumulation in the medium over the next 24 h was measured. Cultured cells from day 12 fetuses secreted about 1 fmol insulin per pancreas in response to 5 or 15 mmol/l glucose irrespective of whether 1 mmol/l tolbutamide, 400 mumol/l diazoxide, 5 mmol/l theophylline or 10 mmol/l mannoheptulose was present. In contrast, insulin released from day 13 cultured cells increased significantly from 3.0 +/- 0.6 to 6.2 +/- 2.2 fmol per pancreas, when the glucose concentration was raised. Tolbutamide increased, diazoxide and mannoheptulose decreased and theophylline had no effect on insulin release. Even more pronounced effects were found on insulin release from day 14 cultured cells, in which theophylline also increased the release. In addition, insulin release from cells from pregnancy day 14 was 75 +/- 16 amol/min per pancreas when the cells were perifused for 15-20 min in the presence of 5 mmol/l glucose within 3 h of isolation. Increasing the glucose concentration to 15 mmol/l or adding tolbutamide increased, whereas diazoxide decreased, insulin release in the freshly isolated cells. The insulin content of rat pancreata from pregnancy day 13 was 0.06 +/- 0.01 pmol per pancreas and increased approximately 10-fold every second day up to 6.7 +/- 0.9 pmol on day 17 of pregnancy. Between day 17 and 19 the pancreatic insulin content increased about fivefold to 39 +/- 2 pmol. The present data suggest that critical components of the insulin-secretory machinery, including ATP-regulated K+ channels, glucokinase and adenylate cyclase activities, are present in the developing beta-cell earlier than hitherto thought.

摘要

在妊娠第12 - 14天从胰腺原基中分离出胎鼠胰腺细胞,并在5 mmol/l葡萄糖存在的情况下培养48小时。测定接下来24小时培养基中胰岛素的积累量。来自妊娠第12天胎儿的培养细胞,无论是否存在1 mmol/l甲苯磺丁脲、400 μmol/l二氮嗪、5 mmol/l茶碱或10 mmol/l甘露庚酮糖,在5或15 mmol/l葡萄糖刺激下,每个胰腺分泌约1 fmol胰岛素。相比之下,当葡萄糖浓度升高时,来自妊娠第13天培养细胞的胰岛素释放量从每个胰腺3.0±0.6 fmol显著增加到6.2±2.2 fmol。甲苯磺丁脲增加胰岛素释放,二氮嗪和甘露庚酮糖减少胰岛素释放,茶碱对胰岛素释放无影响。在来自妊娠第14天培养细胞的胰岛素释放上发现了更显著的效应,其中茶碱也增加了胰岛素释放。此外,在分离后3小时内,当细胞在5 mmol/l葡萄糖存在下进行15 - 20分钟的灌流时,来自妊娠第14天细胞的胰岛素释放量为每个胰腺75±16 amol/分钟。将葡萄糖浓度增加到15 mmol/l或添加甲苯磺丁脲会增加新分离细胞中的胰岛素释放,而二氮嗪则会减少胰岛素释放。妊娠第13天大鼠胰腺的胰岛素含量为每个胰腺0.06±0.01 pmol,并且每隔一天大约增加10倍,直到妊娠第17天达到6.7±0.9 pmol。在第17天至19天之间,胰腺胰岛素含量增加约五倍,达到39±2 pmol。目前的数据表明,胰岛素分泌机制的关键组成部分,包括ATP调节的钾通道、葡萄糖激酶和腺苷酸环化酶活性,在发育中的β细胞中出现的时间比迄今认为的更早。

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