Silver nanoparticles (AgNP) are promising candidates for fighting drug-resistant infections because of their intrinsic antimicrobial effect. The design of high-yield antimicrobial molecules may inadvertently cause variation in host cells’ biological responses. While many factors affect AgNPs’ efficacy, their surface is exposed to the biological environment and thus plays a critical role in both the preservation of antimicrobial efficacy against pathogens and the modulation of host cells cytotoxicity. This work investigated an engineered biomimetic interface approach to controlling AgNP surface properties to provide them a competitive advantage in a biological environment. Here, a fusion protein featuring a silver-binding peptide (AgBP) domain was engineered to enable self-assembly and track assembly by a green fluorescent protein (GFP) reporter. Following AgNP functionalisation with GFP–AgBP, their antimicrobial and cytotoxic properties were evaluated. GFP–AgBP binding affinity to AgNPs was evaluated using localized surface plasmon resonance sensing. The GFP–AgBP biomimetic interface on AgNPs’ surfaces provided sustained antibacterial efficacy at low concentrations based on bacterial growth inhibition assays. Viability and cytotoxicity measurements in fibroblast cells exposed to GFP–AgBP protein-functionalised AgNPs showed significant improvement compared to controls. Biointerface engineering offers promise towards tailoring AgNP antimicrobial efficacy while addressing safety concerns to maintain optimum cellular interactions.
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1 September 2016
Research Article|
October 21 2016
Biosilver nanoparticle interface offers improved cell viability Available to Purchase
Sarah Kay VanOosten, MS;
Sarah Kay VanOosten, MS
PhD Student
Bioengineering Research Center, Department of Bioengineering, University of Kansas, Lawrence, KS, USA
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Esra Yuca, PhD;
Esra Yuca, PhD
Postdoctoral Research Fellow, Research Associate
Bioengineering Research Center, Department of Mechanical Engineering, University of Kansas, Lawrence, KS, USA
Department of Molecular Biology, Yildiz Technical University, Istanbul, Turkey
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Banu Taktak Karaca, PhD;
Banu Taktak Karaca, PhD
Postdoctoral Research Fellow
Bioengineering Research Center, Department of Mechanical Engineering, University of Kansas, Lawrence, KS, USA
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Kyle Boone, MS;
Kyle Boone, MS
PhD Student
Bioengineering Research Center, Department of Bioengineering, University of Kansas, Lawrence, KS, USA
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Malcolm L. Snead, DDS, PhD;
Malcolm L. Snead, DDS, PhD
Professor and Chair
Division of Biomedical Sciences, Center for Craniofacial Molecular Biology, Herman Ostrow School of Dentistry, The University of Southern California, Los Angeles, CA, USA
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Paulette Spencer, DDS, PhD;
Paulette Spencer, DDS, PhD
Ackers Distinguished Professor and Director
Bioengineering Research Center, Department of Mechanical Engineering, University of Kansas, Lawrence, KS, USA
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Candan Tamerler, PhD
Candan Tamerler, PhD
*
Wesley G. Cramer Professor
Bioengineering Research Center, Department of Mechanical Engineering, University of Kansas, Lawrence, KS, USA
*Corresponding author e-mail address: ctamerler@ku.edu
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*Corresponding author e-mail address: ctamerler@ku.edu
Publisher: Emerald Publishing
Received:
July 20 2016
Accepted:
September 26 2016
Online ISSN: 2050-6260
Print ISSN: 2050-6252
ICE Publishing: All rights reserved
2016
Surface Innovations (2016) 4 (3): 121–132.
Article history
Received:
July 20 2016
Accepted:
September 26 2016
Citation
VanOosten SK, Yuca E, Karaca BT, Boone K, Snead ML, Spencer P, Tamerler C (2016), "Biosilver nanoparticle interface offers improved cell viability". Surface Innovations, Vol. 4 No. 3 pp. 121–132, doi: https://doi.org/10.1680/jsuin.16.00010
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