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胰岛淀粉样多肽的生物合成。在小鼠βTC3细胞中表达升高。

Biosynthesis of islet amyloid polypeptide. Elevated expression in mouse beta TC3 cells.

作者信息

Nagamatsu S, Nishi M, Steiner D F

机构信息

Department of Biochemistry, University of Chicago, Illinois 60637.

出版信息

J Biol Chem. 1991 Jul 25;266(21):13737-41.

PMID:1856207
Abstract

Islet amyloid polypeptide (IAPP) messenger RNA levels, biosynthesis, processing, and secretion were studied in cultured mouse beta TC3 insulinoma cells. Northern blot analysis revealed that the size of IAPP mRNA (0.9 kb) in beta TC3 cells was the same as that in normal mouse islets; IAPP mRNA was approximately 60% of the level of insulin mRNA in beta TC3 cells. However, the ratio of synthesis of insulin to IAPP was approximately 6:1, suggesting that IAPP mRNA is not translated efficiently in these cells. Metabolic labeling of beta TC3 cells with [3H]leucine revealed the synthesis of both a precursor form of IAPP (pro-IAPP) of apparent Mr 7400 and a mature form (IAPP) of apparent Mr 3900. In pulse-chase experiments, pro-IAPP could be shown to be processed to IAPP in a manner similar to proinsulin. The t1/2 for conversion of pro-IAPP to IAPP was about 25 min, faster than the t1/2 for proinsulin to insulin of 70 min. A significant proportion of newly synthesized IAPP and insulin precursors were secreted via a constitutive pathway from beta TC3 cells. Possible effects of dexamethasone and forskolin on IAPP mRNA levels and biosynthesis were examined but no effects were observed. In conclusion, the IAPP gene is strongly expressed in beta TC3 cells leading to the biosynthesis, proteolytic processing, and secretion of IAPP, a putative islet hormone.

摘要

在培养的小鼠β TC3胰岛素瘤细胞中研究了胰岛淀粉样多肽(IAPP)的信使核糖核酸水平、生物合成、加工及分泌情况。Northern印迹分析显示,β TC3细胞中IAPP信使核糖核酸(0.9 kb)的大小与正常小鼠胰岛中的相同;IAPP信使核糖核酸水平约为β TC3细胞中胰岛素信使核糖核酸水平的60%。然而,胰岛素与IAPP的合成比例约为6:1,这表明IAPP信使核糖核酸在这些细胞中翻译效率不高。用[3H]亮氨酸对β TC3细胞进行代谢标记显示,合成了表观分子量为7400的IAPP前体形式(前IAPP)和表观分子量为3900的成熟形式(IAPP)。在脉冲追踪实验中,前IAPP可被证明以类似于胰岛素原的方式加工成IAPP。前IAPP转化为IAPP的半衰期约为25分钟,比胰岛素原转化为胰岛素的70分钟半衰期要快。相当一部分新合成的IAPP和胰岛素前体通过组成型途径从β TC3细胞分泌。研究了地塞米松和福斯高林对IAPP信使核糖核酸水平和生物合成的可能影响,但未观察到影响。总之,IAPP基因在β TC3细胞中强烈表达,导致IAPP(一种假定的胰岛激素)的生物合成、蛋白水解加工及分泌。

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