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自动化固相肽合成以获得治疗性肽。

Automated solid-phase peptide synthesis to obtain therapeutic peptides.

机构信息

Institute of Biochemistry, Faculty of Biosciences, Pharmacy and Psychology, Universität Leipzig, Brüderstraße 34, D-04103 Leipzig, Germany.

出版信息

Beilstein J Org Chem. 2014 May 22;10:1197-212. doi: 10.3762/bjoc.10.118. eCollection 2014.

Abstract

The great versatility and the inherent high affinities of peptides for their respective targets have led to tremendous progress for therapeutic applications in the last years. In order to increase the drugability of these frequently unstable and rapidly cleared molecules, chemical modifications are of great interest. Automated solid-phase peptide synthesis (SPPS) offers a suitable technology to produce chemically engineered peptides. This review concentrates on the application of SPPS by Fmoc/t-Bu protecting-group strategy, which is most commonly used. Critical issues and suggestions for the synthesis are covered. The development of automated methods from conventional to essentially improved microwave-assisted instruments is discussed. In order to improve pharmacokinetic properties of peptides, lipidation and PEGylation are described as covalent conjugation methods, which can be applied by a combination of automated and manual synthesis approaches. The synthesis and application of SPPS is described for neuropeptide Y receptor analogs as an example for bioactive hormones. The applied strategies represent innovative and potent methods for the development of novel peptide drug candidates that can be manufactured with optimized automated synthesis technologies.

摘要

在过去的几年中,肽的巨大多功能性和对其各自靶标的固有高亲和力,使得治疗应用取得了巨大进展。为了提高这些通常不稳定且迅速清除的分子的药物可用性,化学修饰具有重要意义。自动化固相肽合成(SPPS)提供了一种生产化学工程肽的合适技术。本综述重点介绍了最常用的 Fmoc/t-Bu 保护基策略的 SPPS 应用。涵盖了合成的关键问题和建议。讨论了从传统到基本改进的微波辅助仪器的自动化方法的发展。为了改善肽的药代动力学特性,脂质化和聚乙二醇化被描述为共价缀合方法,可通过自动化和手动合成方法的组合应用。以神经肽 Y 受体类似物为例,描述了 SPPS 的合成和应用,作为生物活性激素的例子。应用的策略代表了开发新型肽药物候选物的创新和有效方法,这些候选物可以通过优化的自动化合成技术制造。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b0aa/4077397/0d568b587d21/Beilstein_J_Org_Chem-10-1197-g007.jpg

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