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重组DNA技术在糖尿病治疗中的应用:胰岛素类似物

Recombinant DNA technology in the treatment of diabetes: insulin analogs.

作者信息

Vajo Z, Fawcett J, Duckworth W C

机构信息

Section of Endocrinology, VA Medical Center, Phoenix, Arizona 85012, USA.

出版信息

Endocr Rev. 2001 Oct;22(5):706-17. doi: 10.1210/edrv.22.5.0442.

DOI:10.1210/edrv.22.5.0442
PMID:11588149
Abstract

After more than half a century of treating diabetics with animal insulins, recombinant DNA technologies and advanced protein chemistry made human insulin preparations available in the early 1980s. As the next step, over the last decade, insulin analogs were constructed by changing the structure of the native protein with the goal of improving the therapeutic properties of it, because the pharmacokinetic characteristics of rapid-, intermediate-, and long-acting preparations of human insulin make it almost impossible to achieve sustained normoglycemia. The first clinically available insulin analog, lispro, confirmed the hopes by showing that improved glycemic control can be achieved without an increase in hypoglycemic events. Two new insulin analogs, insulin glargine and insulin aspart, have recently been approved for clinical use in the United States, and several other analogs are being intensively tested. Thus, it appears that a rapid acceleration of basic and clinical research in this arena will be seen, which will have direct significance to both patients and their physicians. The introduction of new short-acting analogs and the development of the first truly long-acting analogs and the development of analogs with increased stability, less variability, and perhaps selective action, will help to develop more individualized treatment strategies targeted to specific patient characteristics and to achieve further improvements in glycemic control. Data on the currently available and tested analogs, as well as data on those currently being developed, are reviewed.

摘要

在用动物胰岛素治疗糖尿病患者半个多世纪之后,重组DNA技术和先进的蛋白质化学方法使得人类胰岛素制剂在20世纪80年代初得以问世。接下来,在过去十年里,通过改变天然蛋白质的结构构建胰岛素类似物,目的是改善其治疗特性,因为人胰岛素的速效、中效和长效制剂的药代动力学特征几乎不可能实现持续的血糖正常。首个临床可用的胰岛素类似物赖脯胰岛素证实了人们的期望,即无需增加低血糖事件就能实现更好的血糖控制。两种新的胰岛素类似物,甘精胰岛素和门冬胰岛素,最近已在美国获批用于临床,其他几种类似物也正在进行深入测试。因此,似乎在这个领域基础研究和临床研究将迅速加速,这对患者及其医生都将具有直接意义。新型速效类似物的推出、首个真正长效类似物的开发以及具有更高稳定性、更低变异性且可能具有选择性作用的类似物的开发,将有助于制定针对特定患者特征的更个体化治疗策略,并进一步改善血糖控制。本文综述了目前可用和已测试的类似物的数据,以及目前正在开发的类似物的数据。

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Recombinant DNA technology in the treatment of diabetes: insulin analogs.重组DNA技术在糖尿病治疗中的应用:胰岛素类似物
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