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甘氨酸延伸型胃泌素加工中间体:积累及与胃泌素的共分泌

Glycine-extended progastrin processing intermediates: accumulation and cosecretion with gastrin.

作者信息

Sugano K, Park J, Dobbins W O, Yamada T

机构信息

Department of Internal Medicine, University of Michigan Medical Center, Ann Arbor 48109-0362.

出版信息

Am J Physiol. 1987 Oct;253(4 Pt 1):G502-7. doi: 10.1152/ajpgi.1987.253.4.G502.

Abstract

Glycine-extended intermediates of peptide processing serve as substrates for carboxyl-terminal amidation, hence activation, of many brain-gut peptides. To explore the dynamics of accumulation and secretion of these important intermediates we utilized primary cultures of canine antral mucosal G-cells as a model system. Glycine-extended progastrin processing intermediates (G-Gly) accumulated rapidly in G-cells cultured in ascorbate-deficient media, exhibiting a fourfold increase over a 51-h culture period, while gastrin content fell to less than half of the initial level. In contrast, G-cells cultured in ascorbate-supplemented media accumulated G-Gly at a relatively low rate, while gastrin was preserved at a higher level. Under either condition, G-Gly and gastrin were progressively released into the culture media. The release of both immunoreactivities could be stimulated by bombesin and inhibited by somatostatin in similar fashion. By electron microscopy, the cultured G-cells exhibited no ultrastructural alterations. These data suggest that 1) the cellular homeostasis of G-Gly is regulated by the activity of an ascorbate-dependent amidation enzyme similar to one previously described in pituitary tissues, 2) carboxyl-terminal amidation is not an obligatory step for secretion of gastrin, and 3) the proportions of gastrin and G-Gly cosecreted from G-cells reflect their proportional accumulation within G-cell secretory granules. The physiological relevance of the released G-Gly has yet to be determined.

摘要

肽加工过程中甘氨酸延伸的中间体可作为许多脑肠肽的羧基末端酰胺化底物,从而实现激活。为了探究这些重要中间体的积累和分泌动态,我们利用犬胃窦黏膜G细胞的原代培养物作为模型系统。在缺乏抗坏血酸的培养基中培养的G细胞中,甘氨酸延伸的胃泌素加工中间体(G-Gly)迅速积累,在51小时的培养期内增加了四倍,而胃泌素含量降至初始水平的一半以下。相比之下,在添加抗坏血酸的培养基中培养的G细胞以相对较低的速率积累G-Gly,而胃泌素则保持在较高水平。在任何一种条件下,G-Gly和胃泌素都逐渐释放到培养基中。两种免疫反应性的释放都可以被蛙皮素刺激,并被生长抑素以类似方式抑制。通过电子显微镜观察,培养的G细胞没有表现出超微结构改变。这些数据表明:1)G-Gly的细胞内稳态受一种类似于先前在垂体组织中描述的依赖抗坏血酸的酰胺化酶活性的调节;2)羧基末端酰胺化不是胃泌素分泌的必要步骤;3)从G细胞共分泌的胃泌素和G-Gly的比例反映了它们在G细胞分泌颗粒中的比例积累。释放的G-Gly的生理相关性尚待确定。

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