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Acta BiomaterialiaVolume 10, Issue 8, August 2014, Pages 3513-3521

Characterization of hLF1-11 immobilization onto chitosan ultrathin films, and its effects on antimicrobial activity(Article)

  • aINEB - Instituto de Engenharia Biomédica, Universidade Do Porto, Rua do Campo Alegre 823, 4150-180 Porto, Portugal
  • bUniversidade Do Porto, Faculdade de Engenharia, Porto, Portugal
  • cUniversidade Do Porto, CIQ-UP - Departamento de Química e Bioquímica, Faculdade de Ciências, Porto, Portugal
  • dUniversidade Do Porto, Instituto de Ciências Biomédicas Abel Salazar, Porto, Portugal

Abstract

hLF1-11 (GRRRRSVQWCA) is an antimicrobial peptide (AMP) with high activity against methicillin-resistant Staphylococcus aureus (MRSA), the most prevalent species in implant-associated infection. In this work, the effect of the surface immobilization on hLF1-11 antimicrobial activity was studied. Immobilization was performed onto chitosan thin films as a model for an implant coating due to its reported osteogenic and antibacterial properties. Chitosan thin films were produced by spin-coating on gold surfaces. hLF1-11 was immobilized onto these films by its C-terminal cysteine in an orientation that exposes the antimicrobial activity-related arginine-rich portion of the peptide. Two levels of exposure (with and without a polyethylene glycol (PEG) spacer) were analyzed. Covalent immobilization was further compared with the AMP physical adsorption onto chitosan films. Surfaces were characterized using ellipsometry, contact angle measurements, atomic force microscopy, infrared and X-ray photoelectron spectroscopies and using a fluorimetric assay for hLF1-11 quantification. Surface antimicrobial activity was assessed through surface adhesion and viability assays using an MRSA (S. aureus ATCC 33591). The incorporation of hLF1-11 increased significantly bacterial adhesion to chitosan films. However, the presence of hLF1-11, namely when immobilized through a PEG spacer, decreased the viability of adherent bacteria with regard to the control surface. These results demonstrated that hLF1-11 after covalent immobilization by its cysteine can maintain activity, particularly if a spacer is applied. However, further studies, exploring the opposite orientation or the same C-terminal orientation, but non-cysteine related, can help to clarify the potential of the hLF1-11 immobilization strategy. © 2014 Acta Materialia Inc. Published by Elsevier Ltd. All rights reserved.

Author keywords

Antimicrobial peptides (AMP)Bacterial adhesionChitosanSurface characterizationSurface immobilization

Indexed keywords

EMTREE drug terms:chitosanmacrogolpolypeptide antibiotic agentserine arginine rich proteinantiinfective agentartificial membranebiomaterialchitosanlactoferrinlactoferrin (1-11), humanpeptide fragmentprotein binding
EMTREE medical terms:adsorptionantibacterial activityarticleatomic force microscopybacterium adherencecontact anglecontrolled studydensityellipsometryfluorometryimmobilizationmeasurementmethicillin resistant Staphylococcus aureusnonhumanpriority journalsurface propertyX ray photoelectron spectroscopyartificial membranecell survivalchemistrydrug effectsmaterials testingphysiologysynthesis
Species Index:Bacteria (microorganisms)methicillin resistant Staphylococcus aureusStaphylococcus aureus
MeSH:AdsorptionAnti-Infective AgentsCell SurvivalChitosanCoated Materials, BiocompatibleLactoferrinMaterials TestingMembranes, ArtificialMethicillin-Resistant Staphylococcus aureusPeptide FragmentsProtein Binding

Chemicals and CAS Registry Numbers:

chitosan, 9012-76-4; macrogol, 25322-68-3; lactoferrin, 55599-62-7;

Anti-Infective Agents; Chitosan; Coated Materials, Biocompatible; Lactoferrin; lactoferrin (1-11), human; Membranes, Artificial; Peptide Fragments

Funding details

Funding sponsor Funding number Acronym
Programa Operacional Temático Factores de CompetitividadeCOMPETE
Fundação para a Ciência e a Tecnologia
See opportunities		PTDC/CTM/101484/2008,SFRH/BD/72471/2010,PEst-C/SAU/LA0002/2013
Fundação para a Ciência e a Tecnologia
See opportunities

  • 1

    This work was financed by FEDER funds through the Programa Operacional Factores de Competitividade (COMPETE) and by Portuguese funds through FCT (Fundação para a Ciência e a Tecnologia) in the framework of the projects: PTDC/CTM/101484/2008; PEst-C/SAU/LA0002/2013. Fabíola Costa acknowledges FCT, for the PhD grant SFRH/BD/72471/2010. We acknowledge Manuela Brás from SUIM (INEB) for the AFM studies. Appendix A

  • ISSN: 17427061
  • Source Type: Journal
  • Original language: English
  • DOI: 10.1016/j.actbio.2014.02.028
  • PubMed ID: 24631659
  • Document Type: Article
  • Publisher: Elsevier Ltd

  Martins, M.C.L.; Instituto de Engenharia Biomédica (INEB), Rua do Campo Alegre 823, Portugal;
© Copyright 2014 Elsevier B.V., All rights reserved.

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