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首页> 外文期刊>Journal of cell biology >Newly synthesized proinsulin/insulin and stored insulin are released from pancreatic B cells predominantly via a regulated, rather than a constitutive, pathway.
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Newly synthesized proinsulin/insulin and stored insulin are released from pancreatic B cells predominantly via a regulated, rather than a constitutive, pathway.

机译:新合成的胰岛素原/胰岛素和储存的胰岛素主要通过调节的而非组成性途径从胰腺B细胞释放。

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The pancreatic B cell has been used as a model to compare the release of newly synthesized prohormone/hormone with that of stored hormone. Secretion of newly synthesized proinsulin/insulin (labeled with [3H]leucine during a 5-min pulse) and stored total immunoreactive insulin was monitored from isolated rat pancreatic islets at basal and stimulatory glucose concentrations over 180 min. By 180 min, 15% of the islet content of stored insulin was released at 16.7 mM glucose compared with 2% at 2.8 mM glucose. After a 30-min lag period, release of newly synthesized (labeled) proinsulin and insulin was detected; from 60 min onwards this release was stimulated up to 11-fold by 16.7 mM glucose. At 180 min, 60% of the initial islet content of labeled proinsulin was released at 16.7 mM glucose and 6% at 2.8 mM glucose. Specific radioactivity of the released newly synthesized hormone relative to that of material in islets indicated its preferential release. A similar degree of isotopic enrichment of released, labeled products was observed at both glucose concentrations. Quantitative HPLC analysis of labeled products indicated that glucose had no effect on intracellular proinsulin to insulin conversion; release of both newly synthesized proinsulin and insulin was sensitive to glucose stimulation; 90% of the newly synthesized hormone was released as insulin; and only 0.5% of proinsulin was rapidly released (between 30 and 60 min) in a glucose-independent fashion. It is thus concluded that the major portion of released hormone, whether old or new, processed or unprocessed, is directed through the regulated pathway, and therefore the small (less than 1%) amount released via a constitutive pathway cannot explain the preferential release of newly formed products from the B cell.
机译:胰腺B细胞已用作比较新合成的激素原/激素与储存激素的释放的模型。在180分钟内,从分离的大鼠胰岛中监测新合成的胰岛素原/胰岛素的分泌(在5分钟的脉冲中用[3H]亮氨酸标记)和储存的总免疫反应性胰岛素。到180分钟时,在16.7 mM葡萄糖下释放了15%的储存胰岛素胰岛含量,而在2.8 mM葡萄糖下释放了2%。滞后30分钟后,检测到新合成的(标记的)胰岛素原和胰岛素释放。从60分钟起,此释放被16.7 mM葡萄糖刺激高达11倍。在180分钟时,标记的胰岛素原的初始胰岛含量的60%在16.7 mM葡萄糖时释放,而在2.8 mM葡萄糖时释放6%。相对于胰岛中的物质,所释放的新合成激素的比放射性表明其优先释放。在两个葡萄糖浓度下都观察到释放的标记产物的同位素富集程度相似。标记产品的定量HPLC分析表明,葡萄糖对细胞内胰岛素原向胰岛素的转化没有影响。新合成的胰岛素原和胰岛素的释放均对葡萄糖刺激敏感;新合成的激素中有90%作为胰岛素释放;并且只有0.5%的胰岛素原以不依赖葡萄糖的方式迅速释放(30至60分钟之间)。因此可以得出结论,无论是旧的还是新的,加工的或未加工的激素,其释放的主要部分都是通过调节途径引导的,因此通过组成性途径释放的少量(少于1%)不能解释优先释放的激素。 B细胞新形成的产物。

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