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甲苯磺丁脲预处理对新合成的胰岛素原转化为胰岛素的速率以及分离的大鼠胰岛中胰岛素储存的区室特征的影响。

Effects of tolbutamide pretreatment on the rate of conversion of newly synthesized proinsulin to insulin and the compartmental characteristics of insulin storage in isolated rat islets.

作者信息

Gold G, Pou J, Gishizky M L, Landahl H D, Grodsky G M

出版信息

Diabetes. 1986 Jan;35(1):6-12. doi: 10.2337/diab.35.1.6.

Abstract

Tolbutamide (1 g/kg body wt) was administered to male rats for 3 days to determine the effects of this pretreatment on subsequent insulin biosynthesis and compartmental storage characteristics of freshly isolated islets. Islets were isolated 16 h after the last tolbutamide administration, at a time when fed plasma glucose concentrations were normal. Islet glucagon was unchanged but insulin content was significantly reduced (38 +/- 1.2 ng IRI/islet from seven untreated rats versus 7.9 +/- 1.2 ng IRI/islet from eight treated rats). After tolbutamide pretreatment, the rate of incorporation of 3H-leucine into islet proinsulin was unchanged, but the t1/2 of labeled proinsulin-to-insulin conversion was significantly (P less than 0.001) decreased from 36 to 20 min. After treatment, actual rates of glucose-stimulated insulin secretion were 50% lower, however, because due to the proportionately greater depletion of islet insulin content, the fractional rate of secretion was increased two-fold. After treatment, there was evidence of compartmental, heterogeneous insulin storage, and glucose still marked newly synthesized insulin for preferential release; however, the differential release of new and old insulin converged rapidly with time. Mathematical integration of the data suggested dilution of the newly synthesized insulin compartment with unlabeled insulin during the chase period, but additionally indicated more rapid mixing of newly synthesized with previously stored, unlabeled insulin. Thus, tolbutamide-treated rats partially compensated for acute insulin depletion by increasing the rate of proinsulin-to-insulin conversion, but not increasing the rate of proinsulin biosynthesis; doubling the glucose-stimulated fractional secretory rate of the depleted cellular insulin storage compartment; and retaining compartmental storage characteristics but mixing newly synthesized insulin more rapidly with the compartment of previously stored, unlabeled insulin.

摘要

将甲苯磺丁脲(1克/千克体重)给予雄性大鼠,持续3天,以确定这种预处理对新鲜分离胰岛随后的胰岛素生物合成和区室储存特征的影响。在最后一次给予甲苯磺丁脲16小时后分离胰岛,此时喂食状态下的血浆葡萄糖浓度正常。胰岛胰高血糖素未发生变化,但胰岛素含量显著降低(7只未处理大鼠的胰岛胰岛素含量为38±1.2纳克IRI/胰岛,而8只处理大鼠的胰岛胰岛素含量为7.9±1.2纳克IRI/胰岛)。甲苯磺丁脲预处理后,3H-亮氨酸掺入胰岛胰岛素原的速率未变,但标记的胰岛素原向胰岛素转化的半衰期从36分钟显著(P<0.001)降至20分钟。然而,处理后,葡萄糖刺激的胰岛素实际分泌速率降低了50%,由于胰岛胰岛素含量成比例地更大程度减少,分泌分数率增加了两倍。处理后,有证据表明存在区室化的异质性胰岛素储存,并且葡萄糖仍然标记新合成的胰岛素以便优先释放;然而,新胰岛素和旧胰岛素的差异释放随时间迅速趋同。数据的数学整合表明,在追踪期内新合成的胰岛素区室被未标记的胰岛素稀释,但还表明新合成的胰岛素与先前储存的未标记胰岛素混合得更快。因此,甲苯磺丁脲处理的大鼠通过提高胰岛素原向胰岛素的转化速率,但不提高胰岛素原生物合成速率;使耗尽的细胞胰岛素储存区室的葡萄糖刺激的分泌分数率加倍;并保留区室储存特征,但使新合成的胰岛素与先前储存的未标记胰岛素区室更快混合,从而部分补偿了急性胰岛素耗竭。

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