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胰岛素蛋白酶从胰高血糖素中释放出一个已知对Ca2+ + Mg2+依赖性ATP酶具有增强活性的片段。

Insulin proteinase liberates from glucagon a fragment known to have enhanced activity against Ca2+ + Mg2+-dependent ATPase.

作者信息

Rose K, Savoy L A, Muir A V, Davies J G, Offord R E, Turcatti G

机构信息

Département de Biochimie Médicale, Centre Médical Universitaire, Geneva, Switzerland.

出版信息

Biochem J. 1988 Dec 15;256(3):847-51. doi: 10.1042/bj2560847.

Abstract

We find, contrary to previous reports, that substantial cleavage of glucagon by insulin proteinase occurs at only one region, namely the double-basic sequence -Arg17-Arg18-. Cleavage takes place almost exclusively between these two residues, liberating fragments glucagon-(1-17) and glucagon-(18-29). Others have shown that the fragment glucagon-(19-29) is 1000-fold more efficient compared with intact glucagon, at inhibiting the Ca2+-activated and Mg2+-dependent ATPase activity and the Ca2+ pump of liver plasma membranes. We show that this fragment is not liberated in detectable quantities by our insulin proteinase preparation. On the other hand, others have shown that glucagon-(18-29), though less active than glucagon-(19-29), was still 100-fold more active than glucagon itself in the above-mentioned system. Our observations represent the first demonstration of the release by insulin proteinase of a hormone fragment having enhanced activity, although it has yet to be shown that the activity of this fragment is important in vivo. Since the formation of glucagon-(19-29) from glucagon-(18-29) would involve merely removal of Arg18, a second enzyme might exist to provide the more active fragment.

摘要

我们发现,与之前的报道相反,胰岛素蛋白酶对胰高血糖素的大量切割仅发生在一个区域,即双碱性序列-Arg17-Arg18-。切割几乎只发生在这两个残基之间,释放出片段胰高血糖素-(1-17)和胰高血糖素-(18-29)。其他人已经表明,与完整的胰高血糖素相比,片段胰高血糖素-(19-29)在抑制肝细胞膜的Ca2+激活和Mg2+依赖的ATP酶活性以及Ca2+泵方面的效率要高1000倍。我们发现,我们的胰岛素蛋白酶制剂不会释放出可检测量的该片段。另一方面,其他人已经表明,胰高血糖素-(18-29)虽然比胰高血糖素-(19-29)活性低,但在上述系统中仍比胰高血糖素本身的活性高100倍。我们的观察结果首次证明了胰岛素蛋白酶释放出了一种活性增强的激素片段,尽管尚未证明该片段的活性在体内很重要。由于从胰高血糖素-(18-29)形成胰高血糖素-(19-29)仅涉及去除Arg18,可能存在第二种酶来产生活性更高的片段。

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