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甘氨酸延伸胃泌素片段的生物活性及铁离子结合能力

Biological activity and ferric ion binding of fragments of glycine-extended gastrin.

作者信息

He Hong, Shehan B Philip, Barnham Kevin J, Norton Raymond S, Shulkes Arthur, Baldwin Graham S

机构信息

The University of Melbourne Department of Surgery, Austin Health, Heidelberg, Victoria 3084, Australia.

出版信息

Biochemistry. 2004 Sep 21;43(37):11853-61. doi: 10.1021/bi0495984.

Abstract

Nonamidated gastrins such as progastrin and glycine-extended gastrin17 (Ggly) induce cell proliferation and migration in vitro and colonic mucosal proliferation in vivo. Our earlier NMR study defined the structure of Ggly and showed that ferric ions are essential to its biological activity, with the first binding to Glu7 and the second to Glu8 and Glu9 (Pannequin, J. et al. (2002) J. Biol. Chem. 277, 48602-48609). The aims of this study were to define the minimum biologically active fragment of Ggly and to determine whether ferric ions were also required for its activity. Cell-proliferation studies with Ggly fragments containing the five glutamate residues showed that the nonapeptide LE(5)AYG, the octapeptide LE(5)AY, and the heptapeptides E(5)AY and LE(5)A were fully active and that their activity was dependent on the presence of ferric ions. The activity of the hexapeptides LE(5) and E(5)A and the pentapeptide E(5) was reduced and independent of the presence of iron. The stoichiometry of ferric ion binding to LE(5)AYG, LE(5)AY, and E(5)AY, determined by absorption spectroscopy, was 2 mol/mol. NMR spectroscopy showed that the nonapeptide LE(5)AYG and shorter fragments had no defined structure and that the iron-binding sites differed from those in Ggly. We conclude that, in contrast to amidated gastrins where the C-terminal tetrapeptide is the minimum bioactive fragment, the shortest fully active fragments of Ggly are the heptapeptides LE(5)A and E(5)AY. These observations indicate that extensive proteolytic processing may not completely inactivate Ggly and that bioactive forms that are not detected by current radioimmunoassays may be present in tissues and/or plasma.

摘要

诸如前胃泌素和甘氨酸延伸型胃泌素17(Ggly)等非酰胺化胃泌素在体外可诱导细胞增殖和迁移,在体内可诱导结肠黏膜增殖。我们早期的核磁共振研究确定了Ggly的结构,并表明铁离子对其生物活性至关重要,第一个铁离子与Glu7结合,第二个与Glu8和Glu9结合(Pannequin,J.等人(2002年)《生物化学杂志》277,48602 - 48609)。本研究的目的是确定Ggly的最小生物活性片段,并确定其活性是否也需要铁离子。对含有五个谷氨酸残基的Ggly片段进行的细胞增殖研究表明,九肽LE(5)AYG、八肽LE(5)AY以及七肽E(5)AY和LE(5)A具有完全活性,且它们的活性依赖于铁离子的存在。六肽LE(5)和E(5)A以及五肽E(5)的活性降低,且与铁的存在无关。通过吸收光谱法测定,铁离子与LE(5)AYG、LE(5)AY和E(5)AY的结合化学计量比为2摩尔/摩尔。核磁共振光谱显示,九肽LE(5)AYG和较短片段没有确定的结构,且铁结合位点与Ggly中的不同。我们得出结论,与酰胺化胃泌素中C末端四肽是最小生物活性片段不同,Ggly最短的完全活性片段是七肽LE(5)A和E(5)AY。这些观察结果表明,广泛的蛋白水解加工可能不会使Ggly完全失活,并且组织和/或血浆中可能存在当前放射免疫测定法未检测到的生物活性形式。

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