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Antimicrobial peptide interactions with silica bead supported bilayers and E. coli: buforin II,magainin II,and arenicin
Authors:Ryan W. Davis  Dulce C. Arango  Howland D. T. Jones  Mark H. Van Benthem  David M. Haaland  Susan M. Brozik  Michael B. Sinclair
Affiliation:1. Electronic and Nanostructured Materials, Sandia National Laboratories, Albuquerque, NM, 87185‐0892, USA;2. Biosensors and Nanomaterials, Sandia National Laboratories, Albuquerque, NM, 87185‐0892, USA;3. Biomolecular Analysis and Imaging, Sandia National Laboratories, Albuquerque, NM, 87185‐0892, USA;4. Materials Characterization, Sandia National Laboratories, Albuquerque, NM, 87185‐0892, USA
Abstract:Using the unique quantitative capabilities of hyperspectral confocal microscopy combined with multivariate curve resolution, a comparative approach was employed to gain a deeper understanding of the different types of interactions of antimicrobial peptides (AMPs) with biological membranes and cellular compartments. This approach allowed direct comparison of the dynamics and local effects of buforin II, magainin II, and arenicin with nanoporous silica bead supported bilayers and living E. coli. Correlating between experiments and comparing these responses have yielded several important discoveries for pursuing the underlying biophysics of bacteriocidal specificity and the connection between structure and function in various cellular environments. First, a novel fluorescence method for direct comparison of a model and living system is demonstrated by utilizing the membrane partitioning and environmental sensitivity of propidium iodide. Second, measurements are presented comparing the temporal dynamics and local equilibrium concentrations of the different antimicrobial agents in the membrane and internal matrix of the described systems. Finally, we discuss how the data lead to a deeper understanding of the roles of membrane penetration and permeabilization in the action of these AMPs. Copyright © 2009 European Peptide Society and John Wiley & Sons, Ltd.
Keywords:antimicrobial peptides  biomimetic systems  spectral imaging  supported bilayers  mesoporous silica  multivariate curve resolution  FRET  buforin II  magainin II  arenicin  nanoscale encapsulation  bio‐materials interfaces  nanoporous containment
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