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大鼠肝细胞原代培养物中血红素结合蛋白的合成与分泌。血红素结合蛋白细胞内前体的证明。

Synthesis and secretion of hemopexin in primary cultures of rat hepatocytes. Demonstration of an intracellular precursor of hemopexin.

作者信息

Katz N R, Goldfarb V, Liem H, Muller-Eberhard U

出版信息

Eur J Biochem. 1985 Jan 2;146(1):155-9. doi: 10.1111/j.1432-1033.1985.tb08632.x.

Abstract

Secretion of hemopexin (20% carbohydrate) and its dependence on glycosylation was studied in primary rat hepatocyte cultures in comparison to the secretion of transferrin (5% carbohydrate). In pulse-chase experiments with [35S]methionine half of the labeled hemopexin was secreted in 30 min. By contrast, it took approximately 50 min for secretion of half of the transferrin. Tunicamycin treatment of cultures significantly delayed the secretion of hemopexin but not that of transferrin. During the pulse period a prominent intracellular precursor of hemopexin, smaller than the mature protein, was evident. It is concluded that the extent of glycosylation of a secretory protein is not necessarily a determinant of the transit time required for intracellular processing and secretion. In the case of hemopexin the glycosylation apparently facilitates the secretion although it is not an absolute prerequisite for the exocytosis of this protein.

摘要

与转铁蛋白(5%碳水化合物)的分泌相比,在原代大鼠肝细胞培养物中研究了血红素结合蛋白(20%碳水化合物)的分泌及其对糖基化的依赖性。在用[35S]甲硫氨酸进行的脉冲追踪实验中,一半标记的血红素结合蛋白在30分钟内分泌出来。相比之下,转铁蛋白分泌一半大约需要50分钟。用衣霉素处理培养物显著延迟了血红素结合蛋白的分泌,但没有延迟转铁蛋白的分泌。在脉冲期,明显可见一种比成熟蛋白小的血红素结合蛋白的突出细胞内前体。得出的结论是,分泌蛋白的糖基化程度不一定是细胞内加工和分泌所需转运时间的决定因素。就血红素结合蛋白而言,糖基化显然促进了分泌,尽管它不是该蛋白胞吐作用的绝对先决条件。

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