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含酰胺键的单分散聚乙二醇超过 10000Da。

Amide bond-containing monodisperse polyethylene glycols beyond 10 000 Da.

机构信息

Hubei Province Engineering and Technology Research Center for Fluorinated Pharmaceuticals and School of Pharmaceutical Sciences, Wuhan University, Wuhan 430071, China.

出版信息

Org Biomol Chem. 2016 Aug 16;14(33):7912-9. doi: 10.1039/c6ob01286h.

Abstract

Although monodisperse polyethylene glycols (M-PEGs) above 4000 Da are especially valuable in biomedical applications, their synthesis remains a long-standing challenge. To this end, a peptide-based strategy for such M-PEGs was developed. With macrocyclic sulfates as the key intermediates, a panel of oligoethylene glycol (OEG) containing ω-amino acids were prepared with high efficiency. Through solid phase peptide synthesis (SPPS), these amino acids were conveniently assembled into a series of amide bond-containing M-PEGs with high flexibility in molecular weight and amide density selection. With this strategy, an M-PEG of 10 262 Da was prepared on a gram scale and its biocompatibility was assessed in a mice model.

摘要

虽然分子量超过 4000 Da 的单分散聚乙二醇(M-PEG)在生物医学应用中特别有价值,但它们的合成仍然是一个长期存在的挑战。为此,开发了一种基于肽的此类 M-PEG 的合成方法。以大环硫酸盐为关键中间体,高效制备了一系列含有ω-氨基酸的低聚乙二醇(OEG)。通过固相肽合成(SPPS),这些氨基酸被方便地组装成一系列酰胺键含有的 M-PEG,分子量和酰胺密度选择具有很高的灵活性。通过这种策略,在毫克规模上制备了分子量为 10262 Da 的 M-PEG,并在小鼠模型中评估了其生物相容性。

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