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A brief overview of antimicrobial peptides containing unnatural amino acids and Ligand-based approaches for peptide Ligands

机译:包含非天然氨基酸的抗菌肽的简要概述以及基于配体的肽配体方法

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Antimicrobial Peptides (AMPs) incorporating unnatural Amino Acids have several advantages over naturally occurring AMPs based on factors such as bioavailability, metabolic stability and overall toxicity. Here we discuss the broad spectrum and organism specific bioactivity of unnatural amino acids incorporating AMPs against gram positive organisms such as S. aureus, E. faecium etc, gram negative organisms such as S. typhimurium, K. pneumonia etc and myco-bacterium organisms such as M. ranae. We present comparative bioactivities of these AMPs against ESKAPE organism and select agent organisms such as Y. pesti, B. anthracis etc. The denovo design philosophy involving the three spacers approach with Spacer-1 defining flexibility, Spacer-2 determining overall surface charge density and Spacer-3 defining the conformational flexibility is discussed. The novel approach of differential computation of logP, Solvent-Accessible-Surface-Area, and Molecular Volume employing tripeptides with Gly as reference vis-à-vis various natural and unnatural amino acids, gives access to the estimation of the three important properties in the designed AMPs. An overview of the interaction studies employing Circular Dichroism (CD), Isothermal Titration Calorimetry (ITC) and induced Calcein leakage studies with these AMPs and various cell membranes mimics is presented.
机译:基于诸如生物利用度,代谢稳定性和整体毒性等因素,掺入非天然氨基酸的抗菌肽(AMP)具有优于天然AMP的多个优势。在这里,我们讨论了掺入AMPs的非天然氨基酸对革兰氏阳性生物(如金黄色葡萄球菌,粪肠球菌等),革兰氏阴性生物(如鼠伤寒沙门氏菌,肺炎克雷伯氏菌等)和分枝杆菌生物等的广谱和生物特异性生物活性。如M. ranae。我们介绍了这些AMPs对ESKAPE生物体和选择的病原体生物体(如Y.pesti,B.anthracis等)的比较生物活性。denovo设计原理涉及三个间隔子方法,其中Spacer-1定义了柔韧性,Spacer-2确定了整体表面电荷密度和讨论了限定构象柔性的间隔物3。使用三肽和Gly作为参比,对各种天然和非天然氨基酸进行logP,溶剂可及表面面积和分子体积的微分计算的新颖方法,提供了对三种重要特性的估算方法设计的AMP。概述了使用圆二色谱(CD),等温滴定热量法(ITC)以及与这些AMP和各种细胞膜模拟物诱导的钙黄绿素泄漏研究的相互作用研究。

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