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理解蛋白酶催化的固相肽合成。

Understanding protease catalysed solid phase peptide synthesis.

作者信息

Ulijn Rein V, Bisek Nicola, Halling Peter J, Flitsch Sabine L

机构信息

Department of Chemistry, University of Edinburgh, King's Buildings, West Mains Road, Edinburgh, Scotland, UK EH9 3JJ.

出版信息

Org Biomol Chem. 2003 Apr 21;1(8):1277-81. doi: 10.1039/b211890d.

Abstract

A protease (thermolysin) was used to directly synthesise a number of dipeptides from soluble Fmoc-amino acids onto a solid support (PEGA1900) in bulk aqueous media, often in very good yields. This shift in equilibrium toward synthesis is remarkable because for soluble dipeptides in aqueous solution hydrolysis rather than synthesis is observed. Three possible reasons for the equilibrium shift were considered: (i) using a solid support makes it easy to use an excess of reagents, so mass action contributes towards synthesis; (ii) reduction in the unfavourable hydrophobic hydration of the Fmoc group within the solid support compared with the free amino acid in solution and (iii) suppression of the ionization of amino groups linked to the solid phase due to mutual electrostatic repulsion. It was found that under the conditions studied the second effect was most important.

摘要

一种蛋白酶(嗜热菌蛋白酶)被用于在大量水性介质中,从可溶性芴甲氧羰基氨基酸(Fmoc-氨基酸)直接在固体载体(PEGA1900)上合成多种二肽,产率通常很高。这种平衡向合成方向的转变很显著,因为在水溶液中,可溶性二肽会发生水解而非合成。人们考虑了平衡转变的三个可能原因:(i)使用固体载体便于使用过量试剂,因此质量作用有助于合成;(ii)与溶液中的游离氨基酸相比,固体载体内芴甲氧羰基(Fmoc)基团不利的疏水水合作用减弱;(iii)由于相互静电排斥,抑制了与固相相连的氨基的电离。结果发现,在所研究的条件下,第二种效应最为重要。

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