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胰岛素瘤细胞系中胰岛素相关肽的加工与分泌

Processing and secretion of insulin-related peptides in an insulinoma cell line.

作者信息

Grampp G E, Lodish H F, Stephanopoulos G

机构信息

Department of Chemical Engineering and Bioprocess Engineering Center, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139, USA.

出版信息

Biotechnol Bioeng. 1997 Feb 5;53(3):283-9. doi: 10.1002/(SICI)1097-0290(19970205)53:3<283::AID-BIT6>3.0.CO;2-E.

Abstract

Certain classes of prohormones and other neuroendocrine or endocrine-derived secretory proteins are post-translationally modified in the secretory storage granules. If such molecules were to be biosynthesized to acceptable quantity and yield using endocrine-derived cell lines, it would be important to understand the relationship between the secretory dynamics and the conversion and release of the immature and mature forms of the molecule. We studied aspects of such a relationship using the endocrine-derived cell line betaTC-3, which synthesizes murine proinsulin, sequesters it into secretory granules, and converts it into mature insulin. In T-flask experiments with confluent cultures of betaTC-3 cells, intracellular and secreted (pro)insulin was sampled before and after episodes of stimulated exocytosis and recharging and quantified by radioimmunoassay and reversed-phase high-performance liquid chromatography (HPLC). Under conditions of steady-state secretion in glucose-rich growth medium the cells turned over their (pro)insulin inventory (90 +/- 5% mature insulin) at 2-3% per hour through secretion of (pro)insulin which was less than 70% mature. During an episode of hyperstimulated exocytosis induced by the combined secretagogues carbachol (1 microM) and isobutylmethylxanthine (1 mM), approximately 80% of the intracellular (pro)insulin stores were depleted within 2 h and 84 +/- 4% of the secreted (pro)insulin was in the mature form. Following the discharging episode, exocytosis was suppressed to 10% of its steady-state rate with a treatment which attenuated calcium influx (20 microM verapamil with reduced levels of calcium in the medium). Under this condition the secreted protein was only approximately 50% converted to mature insulin, but 85 +/- 10% of the net (pro)insulin accumulating within the intracellular stores was converted to the mature form. The inverse relationship between rate of secretion and degree of conversion of secreted (pro)insulin is consistent with a previously observed phenomenon of preferential basal secretion from immature secretory granules. This tends to enrich the secreted peptides in immature forms relative to the total intracellular pool. Preferential early secretion can best be overcome by rapid discharging of the long-term and predominantly mature stores. Thus, a cyclic controlled secretion process wherein product is collected during intermittent discharging episodes would provide a better yield of mature product than would steady-state secretion.

摘要

某些类别的激素原以及其他神经内分泌或内分泌衍生的分泌蛋白在分泌储存颗粒中进行翻译后修饰。如果要使用内分泌衍生的细胞系以可接受的数量和产量生物合成此类分子,那么了解分泌动力学与该分子未成熟形式和成熟形式的转化及释放之间的关系就很重要。我们使用内分泌衍生的细胞系betaTC - 3研究了这种关系的各个方面,该细胞系合成小鼠胰岛素原,将其隔离到分泌颗粒中,并将其转化为成熟胰岛素。在对betaTC - 3细胞汇合培养物进行的T型瓶实验中,在刺激的胞吐作用和再填充前后对细胞内和分泌的(原)胰岛素进行取样,并通过放射免疫测定和反相高效液相色谱(HPLC)进行定量。在富含葡萄糖的生长培养基中稳态分泌的条件下,细胞通过分泌成熟度低于70%的(原)胰岛素,以每小时2 - 3%的速度周转其(原)胰岛素库存(90±5%为成熟胰岛素)。在由卡巴胆碱(1 microM)和异丁基甲基黄嘌呤(1 mM)联合促分泌剂诱导的超刺激胞吐作用期间,约80%的细胞内(原)胰岛素储存库在2小时内耗尽,分泌的(原)胰岛素中有84±4%为成熟形式。在释放期之后,通过减弱钙内流的处理(20 microM维拉帕米并降低培养基中的钙水平),胞吐作用被抑制到其稳态速率的10%。在此条件下,分泌的蛋白质仅有约50%转化为成熟胰岛素,但细胞内储存库中积累净(原)胰岛素的85±10%转化为成熟形式。分泌的(原)胰岛素分泌速率与转化程度之间的反比关系与先前观察到的未成熟分泌颗粒优先基础分泌现象一致。这往往会使分泌的肽相对于细胞内总库而言以未成熟形式富集。通过快速排出长期且主要是成熟的储存库,可最好地克服优先早期分泌。因此,与稳态分泌相比,一种周期性控制的分泌过程,即在间歇性释放期收集产物,将能提供更高产量的成熟产物。

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