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高温下难合成肽序列的固相合成:微波加热与传统加热技术的关键比较

Solid-phase synthesis of difficult peptide sequences at elevated temperatures: a critical comparison of microwave and conventional heating technologies.

作者信息

Bacsa Bernadett, Horváti Kata, Bõsze Szilvia, Andreae Fritz, Kappe C Oliver

机构信息

Christian Doppler Laboratory for Microwave Chemistry and Institute of Chemistry, Karl-Franzens-University Graz, Heinrichstrasse 28, A-8010 Graz, Austria.

出版信息

J Org Chem. 2008 Oct 3;73(19):7532-42. doi: 10.1021/jo8013897. Epub 2008 Aug 27.

Abstract

The Fmoc/t-Bu solid-phase synthesis of three difficult peptide sequences (a 9-mer, 15-mer, and 24-mer) was performed using N,N'-diisopropylcarbodiimide/1-hydroxybenzotriazole as coupling reagent on polystyrene, Tentagel, and ChemMatrix resins. In order to obtain an insight into the specific role of the elevated temperature and/or the electromagnetic field for peptide syntheses carried out using microwave irradiation, peptide couplings and Fmoc-deprotection steps were studied under microwave and conventionally heated conditions at the same temperature. While room temperature couplings/deprotections generally produced the difficult peptides in rather poor quality, excellent peptide purities were obtained using microwave heating at a temperature of 86 degrees C for both the coupling and deprotection steps in only 10 and 2.5 min reaction time, respectively. While for most amino acids no significant racemization was observed, the high coupling temperatures led to considerable levels of racemization for the sensitive amino acids His and Cys. It was demonstrated for all three peptide sequences that when performing the coupling/deprotection steps at the same reaction temperature using conventional heating, nearly identical results in terms of both peptide purity and racemization levels were obtained. It therefore appears that the main effect of microwave irradiation applied to solid-phase peptide synthesis is a purely thermal effect not related to the electromagnetic field.

摘要

使用N,N'-二异丙基碳二亚胺/1-羟基苯并三唑作为偶联剂,在聚苯乙烯、Tentagel和ChemMatrix树脂上进行了三种难合成肽序列(9肽、15肽和24肽)的Fmoc/t-Bu固相合成。为了深入了解高温和/或电磁场在微波辐射肽合成中的具体作用,研究了在相同温度下微波和常规加热条件下的肽偶联和Fmoc脱保护步骤。虽然室温下的偶联/脱保护通常会产生质量相当差的难合成肽,但在86℃的温度下,仅分别在10分钟和2.5分钟的反应时间内,通过微波加热进行偶联和脱保护步骤,就获得了优异的肽纯度。虽然对于大多数氨基酸未观察到明显的消旋化,但高偶联温度导致敏感氨基酸组氨酸和半胱氨酸出现相当程度的消旋化。对于所有三个肽序列都证明,当使用常规加热在相同反应温度下进行偶联/脱保护步骤时,在肽纯度和消旋化水平方面都获得了几乎相同的结果。因此,似乎应用于固相肽合成的微波辐射的主要作用是纯粹的热效应,与电磁场无关。

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