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基于 Fmoc 的改进固相合成法用于合成人源和鼠源朊病毒蛋白同源肽段。

Improved Fmoc-based solid-phase synthesis of homologous peptide fragments of human and mouse prion proteins.

机构信息

Institute for Research in Biomedicine, Barcelona Science Park, Baldiri Reixac 10, E-08028 Barcelona, Spain.

出版信息

J Pept Sci. 2011 Jan;17(1):32-8. doi: 10.1002/psc.1293. Epub 2010 Sep 16.

Abstract

The synthesis of difficult peptide sequences has been a challenge since the very beginning of SPPS. The self-assembly of the growing peptide chains has been proposed as one of the causes of this synthetic problem. However, there is an increasing need to obtain peptides and proteins that are prone to aggregate. These peptides and proteins are generally associated with diseases known as amyloidoses. We present an efficient SPPS of two homologous peptide fragments of HuPrP (106-126) and MoPrP105-125 based on the use of the PEGA resin combined with proper coupling approaches. These peptide fragments were also studied by CD and TEM to determine their ability to aggregate. On the basis of these results, we support PEG-based resins as an efficient synthetic tool to prepare peptide sequences prone to aggregate on-resin.

摘要

自固相多肽合成(SPPS)诞生以来,合成困难的肽序列一直是一个挑战。有人提出,不断增长的肽链的自组装是造成这一合成问题的原因之一。然而,人们越来越需要获得容易聚集的肽和蛋白质。这些肽和蛋白质通常与被称为淀粉样变性的疾病有关。我们提出了一种基于使用 PEGA 树脂结合适当偶联方法的有效固相多肽合成 HuPrP(106-126)和 MoPrP105-125 两个同源肽片段的方法。我们还通过 CD 和 TEM 研究了这些肽片段,以确定它们聚集的能力。基于这些结果,我们支持基于 PEG 的树脂作为一种有效的合成工具,用于在树脂上制备容易聚集的肽序列。

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