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T4 lysozyme fused with cellulose-binding module for antimicrobial cellulosic wound dressing materials

机译:T4溶菌酶与纤维素结合模块融合用于抗微生物纤维素伤口敷料材料

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Aims: Bacterial infection is a major challenge in wound care. Antimicrobial wound dressings are of great value for treating wound infections. Endolysins are evolving as a new class of antimicrobials with multiple applications. This study describes the production and evaluation of T4 lysozyme (T4Lyz), product of gene e of the T4 bacteriophage, fused with Cellulose Binding Module (CBM) for facile immobilization to cellulosic wound dressing. Methods and Results: Genes encoding T4Lyz-CBM and T4Lyz were cloned and expressed in Escherichia coli and the enzymes were purified by cation exchange chromatography. While the CBM tag did not alter the optimum pH and stability features of T4Lyz, the lytic activity of the fusion protein was lowered. The bactericidal activity of T4Lyz-CBM, determined by viable count plating assay after 1 h incubation with Micrococcus lysodeikticus was 97·5% with 10 μg ml-1, and 99·96% and 95% for E. coli and Pseudomonas mendocina, respectively, with 200 μg ml-1 enzyme. T4Lyz-CBM was immobilized to wound dressing gauze with a capacity of 5·5 μg mg-1 matrix, whereas the unmodified T4Lyz did not exhibit any binding. The immobilized protein retained its bactericidal activity against Gram-positive and Gram-negative bacteria. Both free and immobilized T4Lyz-CBM, after heat denaturation, retained their bactericidal activities against Gram-negative bacteria only. The immobilized enzyme exhibited higher stability than the free enzyme when stored in dry form or in the presence of polyol stabilizers. Conclusion: Tagging T4Lyz with CBM provides a facile, irreversible binding to cellulosic wound dressing while retaining its activity. This approach may be suitable even for other antimicrobial enzymes and -peptides. Significance and Impact of the Study: The spread of antibiotic resistance requires innovative strategies for discovery and development of effective antimicrobial alternatives. This report presents a novel strategy for producing antimicrobial wound dressing materials.
机译:目的:细菌感染是伤疤中的主要挑战。抗微生物伤口敷料对治疗伤口感染具有很大的价值。 Endolysins正在作为具有多种应用的新一类抗微生物而发展。该研究描述了T4溶菌酶(T4Lyz)的生产和评估,T4噬菌体的基因E产品,与纤维素结合模块(CBM)融合,用于纤维素伤口敷料的体内固定化。方法和结果:在大肠杆菌中克隆并表达编码T4Lyz-CBM和T4的基因,并通过阳离子交换色谱纯化酶。虽然CBM标签没有改变T4LYZ的最佳pH和稳定性特征,但融合蛋白的裂解活性降低。通过分别的1小时孵育1小时后通过可行的计数电镀测定法测定的T4Lyz-CBM的杀菌活性为97·5%,分别为10μgmL-1,99·96%和95%,分别为99·96%和95%的Mendocina ,200μgml-1酶。将T4LYZ-CBM固定在容量为5·5μg-1基质的伤口敷料纱布上,而未修饰的T4LYZ没有表现出任何结合。固定化蛋白质保留其抗革兰氏阳性和革兰氏阴性细菌的杀菌活性。在热变性后,自由和固定的T4LYZ-CBM仅保留其杀菌活性对革兰氏阴性细菌的杀菌活性。当储存在干燥形式或多元醇稳定剂存在时,固定化酶表现出比游离酶更高的稳定性。结论:用CBM标记T4Lyz提供与纤维素伤口敷料的容易,不可逆的结合,同时保留其活性。即使对于其他抗微生物酶和份数,这种方法也可能是合适的。研究的意义和影响:抗生素抗性的传播需要创新的发现和发展有效抗微生物替代品。本报告提出了一种生产抗微生物伤口敷料材料的新策略。

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