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生物科技胰岛素类似物的新时代。

The new era of biotech insulin analogues.

作者信息

Brange J

机构信息

Novo Nordisk A/S, Bagsvaerd, Denmark.

出版信息

Diabetologia. 1997 Jul;40 Suppl 2:S48-53. doi: 10.1007/s001250051400.

Abstract

Many of the structural properties of insulin have evolved in response to the requirements of biosynthesis, processing, transport and storage in the pancreatic beta cells, properties that are not necessary for the biological action of the hormone. It is therefore not surprising that wild-type insulin has far from optimal characteristics for replacement therapy. For example, native human insulin self-associates to hexameric units, which limits the possibilities for the absorption of the molecule by various routes. During the last decade new techniques of molecular design have emerged and recombinant DNA technology offers new and exciting opportunities for rational protein drug design. This review describes examples of recent advances in insulin engineering aimed at optimizing the hormone for therapy. Such approaches focus on improvements in the pharmacokinetic properties, storage stability, and feasibility for less intrusive routes of administration.

摘要

胰岛素的许多结构特性是为了响应胰腺β细胞中生物合成、加工、运输和储存的需求而进化的,而这些特性对于该激素的生物学作用并非必需。因此,野生型胰岛素在替代疗法方面远非具有最佳特性也就不足为奇了。例如,天然人胰岛素会自缔合成六聚体单元,这限制了该分子通过各种途径吸收的可能性。在过去十年中,出现了新的分子设计技术,重组DNA技术为合理的蛋白质药物设计提供了新的、令人兴奋的机会。这篇综述描述了胰岛素工程学最近取得的进展实例,旨在优化该激素用于治疗。此类方法侧重于改善药代动力学特性、储存稳定性以及采用侵入性较小的给药途径的可行性。

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