修饰对环环肽A及其类似物在动物实验模型中免疫抑制特性的影响

Effects of Modifications on the Immunosuppressive Properties of Cyclolinopeptide A and Its Analogs in Animal Experimental Models.

作者信息

Zimecki Michał, Kaczmarek Krzysztof

机构信息

Laboratory of Immunobiology, Hirszfeld Institute of Immunology and Experimental Therapy, Polish Academy of Sciences, R. Weigla Str. 12, 53-114 Wrocław, Poland.

Institute of Organic Chemistry, Lodz University of Technology, S. Żeromskiego Str. 116, 90-924 Łódź, Poland.

出版信息

Molecules. 2021 Apr 27;26(9):2538. doi: 10.3390/molecules26092538.

DOI:10.3390/molecules26092538

PMID:33925288

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8123640/

Abstract

The consequences of manipulations in structure and amino acid composition of native cyclolinopeptide A (CLA) from linen seeds, and its linear precursor on their biological activities and mechanisms of action, are reviewed. The modifications included truncation of the peptide chain, replacement of amino acid residues with proteinogenic or non-proteinogenic ones, modifications of peptide bond, and others. The studies revealed changes in the immunosuppressive potency of these analogs investigated in a number of in vitro and in vivo experimental models, predominantly in rodents, as well as differences in their postulated mechanism of action. The modified peptides were compared with cyclosporine A and parent CLA. Some of the synthesized and investigated peptides show potential therapeutic usefulness.

摘要

本文综述了亚麻籽中天然环亚麻肽A（CLA）及其线性前体的结构和氨基酸组成的操纵对其生物活性和作用机制的影响。这些修饰包括肽链的截短、用蛋白质原性或非蛋白质原性氨基酸残基替代、肽键修饰等。研究揭示了在一些体外和体内实验模型（主要是在啮齿动物中）中研究的这些类似物的免疫抑制效力的变化，以及它们假定的作用机制的差异。将修饰后的肽与环孢素A和母体CLA进行了比较。一些合成和研究的肽显示出潜在的治疗用途。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e49b/8123640/b7d7b8602a43/molecules-26-02538-g001.jpg

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Effects of Modifications on the Immunosuppressive Properties of Cyclolinopeptide A and Its Analogs in Animal Experimental Models.修饰对环环肽A及其类似物在动物实验模型中免疫抑制特性的影响

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修饰对环环肽A及其类似物在动物实验模型中免疫抑制特性的影响

Effects of Modifications on the Immunosuppressive Properties of Cyclolinopeptide A and Its Analogs in Animal Experimental Models.

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