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金属硫蛋白-胰高血糖素融合基因表达的前胰高血糖素的细胞特异性翻译后加工

Cell-specific post-translational processing of preproglucagon expressed from a metallothionein-glucagon fusion gene.

作者信息

Drucker D J, Mojsov S, Habener J F

出版信息

J Biol Chem. 1986 Jul 25;261(21):9637-43.

PMID:3525530
Abstract

Glucagon is a peptide hormone of 29 amino acids encoded by a preprohormone which contains in tandem the sequences of glucagon and two additional glucagon-like peptides (GLPs) structurally related to glucagon and separated by intervening peptides. Glucagon arises by cleavage from the prohormone within the A cells of the pancreatic islets but in the intestine remains as part of a partially processed precursor (glicentin). To determine whether additional glucagon-like peptides are processed from preproglucagon and to analyze for potential cellular specificity in the processing of preproglucagon, we introduced and expressed a metallothionein-glucagon fusion gene in a fibroblast and two endocrine (pituitary and pancreatic islet) cell lines. Chromatographic analyses of cell extracts utilizing specific radioimmunoassays to chemically synthesized peptides demonstrate the liberation of intact glucagon, glicentin, GLP-I(1-37), GLP-I(7-37), GLP-II, and an intervening peptide amidated at its carboxyl terminus. The peptides were present in distinct yet different patterns in the two endocrine but not the fibroblast cell lines. The cell-specific liberation of the glucagon-like and intervening peptides suggests their potential as new bioactive peptides. The cellular specificity in the processing of preproglucagon indicates that the genetic determinants of the processing activity are complex and are expressed in a cell-specific manner.

摘要

胰高血糖素是一种由前激素原编码的29个氨基酸的肽类激素,该前激素原串联包含胰高血糖素的序列以及另外两种与胰高血糖素结构相关的胰高血糖素样肽(GLP),并由间隔肽分隔。胰高血糖素是由胰岛A细胞内的前激素裂解产生的,但在肠道中它仍然是部分加工前体(肠胰高血糖素)的一部分。为了确定是否从前胰高血糖素中加工出其他胰高血糖素样肽,并分析前胰高血糖素加工过程中的潜在细胞特异性,我们在成纤维细胞和两种内分泌(垂体和胰岛)细胞系中导入并表达了金属硫蛋白 - 胰高血糖素融合基因。利用针对化学合成肽的特异性放射免疫测定法对细胞提取物进行色谱分析,结果表明完整的胰高血糖素、肠胰高血糖素、GLP - I(1 - 37)、GLP - I(7 - 37)、GLP - II以及一种在其羧基末端酰胺化的间隔肽被释放出来。这些肽在两种内分泌细胞系中呈现出不同但独特的模式,而成纤维细胞系中则没有。胰高血糖素样肽和间隔肽的细胞特异性释放表明它们有可能成为新的生物活性肽。前胰高血糖素加工过程中的细胞特异性表明,加工活性的遗传决定因素很复杂,并且以细胞特异性方式表达。

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