Staphylococcus aureus Adhesion on Hydrophobin Coatings: Adhesion Forces and the Influence of Surface Charge

Friederike Nolle; Ben Wieland; Kirstin Kochems; Hannah Heintz; Michael Lienemann; Philipp Jung; Hendrik Hähl; Markus Bischoff; Karin Jacobs

doi:10.1021/acsomega.4c11010

Staphylococcus aureus Adhesion on Hydrophobin Coatings: Adhesion Forces and the Influence of Surface Charge

Friederike Nolle
, Ben Wieland
, Kirstin Kochems
, Hannah Heintz
, Michael Lienemann
, Philipp Jung
, Hendrik Hähl
, Markus Bischoff
, Karin Jacobs^*

^*Corresponding author for this work

BA5304 Enzyme and material biotechnology

Saarland University
University of Trier
Oy Medix Biochemica Ab
Max Planck School Matter to Life

Research output: Contribution to journal › Article › Scientific › peer-review

1 Citation (Scopus)

Abstract

Staphylococcus aureus (S. aureus) is one of the bacterial species capable of forming multilayered biofilms on implants. Such biofilms formed on implanted medical devices often require the removal of the implant in order to avoid sepsis or, in the worst case, even the death of the patient. To address the problem of unwanted S. aureus biofilm formation, its first step, i.e., adhesion, must be understood and prevented. Thus, the development of adhesion-reducing surface coatings for implant materials is of utmost importance. In this work, we used single-cell force spectroscopy to analyze the adhesion of the biofilm-forming S. aureus strain SA113 on naive and protein-coated silicon surfaces (SiO₂). In addition to the wild type, we used the SA113 ΔdltA knockout mutant to further investigate the effect of d-alanylation of lipoteichoic acids of the cell wall. In order to examine how the surface charge affects adhesion, we coated silanized SiO₂surfaces with amphiphilic class II hydrophobins. The naturally occurring hydrophobin HFBI was used as well as the HFBI variant D40Q/D43N, which is less negatively charged at physiological pH due to the exchange of two acidic aspartate residues. These two types of hydrophobin-coated surfaces resemble each other in roughness and wettability but differ only in charge. By measurement of the forces with which each S. aureus strain binds to hydrophobin-coated surfaces, we show that the adhesion of S. aureus at surfaces can be influenced by the charges exposed by the target surfaces. Therefore, in addition to hydrogen bonding, electrostatic interactions between the cell and the hydrophilic surface govern adhesion on these surfaces. Moreover, we found that for both HFBI coatings, the adhesion strength of S. aureus is reduced by nearly a factor of 30 compared to silanized SiO₂surfaces. Therefore, hydrophobin coatings are of great interest for further use in the field of biomedical surface coating.

Original language	English
Pages (from-to)	38376-38384
Number of pages	9
Journal	ACS Omega
Volume	10
Issue number	34
DOIs	https://doi.org/10.1021/acsomega.4c11010
Publication status	Published - 2 Sept 2025
MoE publication type	A1 Journal article-refereed

Funding

This research was supported by the German Research Foundation (SFB 1027 B1 and B2, large instrument funding under grant number INST 256/542-1 FUGG, project number 449375068, and large instrument funding under grant number INST 256/583-1 FUGG, project number 519828155) and the Research Council of Finland through an Academy Research Fellowship grant awarded to M.L. (decision no. 321723). K.J. acknowledges funding by the German Federal Ministry of Education and Research (BMBF) by the Max Planck School Matter to Life.

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10.1021/acsomega.4c11010

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title = "Staphylococcus aureus Adhesion on Hydrophobin Coatings: Adhesion Forces and the Influence of Surface Charge",

abstract = "Staphylococcus aureus (S. aureus) is one of the bacterial species capable of forming multilayered biofilms on implants. Such biofilms formed on implanted medical devices often require the removal of the implant in order to avoid sepsis or, in the worst case, even the death of the patient. To address the problem of unwanted S. aureus biofilm formation, its first step, i.e., adhesion, must be understood and prevented. Thus, the development of adhesion-reducing surface coatings for implant materials is of utmost importance. In this work, we used single-cell force spectroscopy to analyze the adhesion of the biofilm-forming S. aureus strain SA113 on naive and protein-coated silicon surfaces (SiO2). In addition to the wild type, we used the SA113 ΔdltA knockout mutant to further investigate the effect of d-alanylation of lipoteichoic acids of the cell wall. In order to examine how the surface charge affects adhesion, we coated silanized SiO2surfaces with amphiphilic class II hydrophobins. The naturally occurring hydrophobin HFBI was used as well as the HFBI variant D40Q/D43N, which is less negatively charged at physiological pH due to the exchange of two acidic aspartate residues. These two types of hydrophobin-coated surfaces resemble each other in roughness and wettability but differ only in charge. By measurement of the forces with which each S. aureus strain binds to hydrophobin-coated surfaces, we show that the adhesion of S. aureus at surfaces can be influenced by the charges exposed by the target surfaces. Therefore, in addition to hydrogen bonding, electrostatic interactions between the cell and the hydrophilic surface govern adhesion on these surfaces. Moreover, we found that for both HFBI coatings, the adhesion strength of S. aureus is reduced by nearly a factor of 30 compared to silanized SiO2surfaces. Therefore, hydrophobin coatings are of great interest for further use in the field of biomedical surface coating.",

author = "Friederike Nolle and Ben Wieland and Kirstin Kochems and Hannah Heintz and Michael Lienemann and Philipp Jung and Hendrik H{\"a}hl and Markus Bischoff and Karin Jacobs",

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T1 - Staphylococcus aureus Adhesion on Hydrophobin Coatings

T2 - Adhesion Forces and the Influence of Surface Charge

AU - Nolle, Friederike

AU - Wieland, Ben

AU - Kochems, Kirstin

AU - Heintz, Hannah

AU - Lienemann, Michael

AU - Jung, Philipp

AU - Hähl, Hendrik

AU - Bischoff, Markus

AU - Jacobs, Karin

PY - 2025/9/2

Y1 - 2025/9/2

N2 - Staphylococcus aureus (S. aureus) is one of the bacterial species capable of forming multilayered biofilms on implants. Such biofilms formed on implanted medical devices often require the removal of the implant in order to avoid sepsis or, in the worst case, even the death of the patient. To address the problem of unwanted S. aureus biofilm formation, its first step, i.e., adhesion, must be understood and prevented. Thus, the development of adhesion-reducing surface coatings for implant materials is of utmost importance. In this work, we used single-cell force spectroscopy to analyze the adhesion of the biofilm-forming S. aureus strain SA113 on naive and protein-coated silicon surfaces (SiO2). In addition to the wild type, we used the SA113 ΔdltA knockout mutant to further investigate the effect of d-alanylation of lipoteichoic acids of the cell wall. In order to examine how the surface charge affects adhesion, we coated silanized SiO2surfaces with amphiphilic class II hydrophobins. The naturally occurring hydrophobin HFBI was used as well as the HFBI variant D40Q/D43N, which is less negatively charged at physiological pH due to the exchange of two acidic aspartate residues. These two types of hydrophobin-coated surfaces resemble each other in roughness and wettability but differ only in charge. By measurement of the forces with which each S. aureus strain binds to hydrophobin-coated surfaces, we show that the adhesion of S. aureus at surfaces can be influenced by the charges exposed by the target surfaces. Therefore, in addition to hydrogen bonding, electrostatic interactions between the cell and the hydrophilic surface govern adhesion on these surfaces. Moreover, we found that for both HFBI coatings, the adhesion strength of S. aureus is reduced by nearly a factor of 30 compared to silanized SiO2surfaces. Therefore, hydrophobin coatings are of great interest for further use in the field of biomedical surface coating.

AB - Staphylococcus aureus (S. aureus) is one of the bacterial species capable of forming multilayered biofilms on implants. Such biofilms formed on implanted medical devices often require the removal of the implant in order to avoid sepsis or, in the worst case, even the death of the patient. To address the problem of unwanted S. aureus biofilm formation, its first step, i.e., adhesion, must be understood and prevented. Thus, the development of adhesion-reducing surface coatings for implant materials is of utmost importance. In this work, we used single-cell force spectroscopy to analyze the adhesion of the biofilm-forming S. aureus strain SA113 on naive and protein-coated silicon surfaces (SiO2). In addition to the wild type, we used the SA113 ΔdltA knockout mutant to further investigate the effect of d-alanylation of lipoteichoic acids of the cell wall. In order to examine how the surface charge affects adhesion, we coated silanized SiO2surfaces with amphiphilic class II hydrophobins. The naturally occurring hydrophobin HFBI was used as well as the HFBI variant D40Q/D43N, which is less negatively charged at physiological pH due to the exchange of two acidic aspartate residues. These two types of hydrophobin-coated surfaces resemble each other in roughness and wettability but differ only in charge. By measurement of the forces with which each S. aureus strain binds to hydrophobin-coated surfaces, we show that the adhesion of S. aureus at surfaces can be influenced by the charges exposed by the target surfaces. Therefore, in addition to hydrogen bonding, electrostatic interactions between the cell and the hydrophilic surface govern adhesion on these surfaces. Moreover, we found that for both HFBI coatings, the adhesion strength of S. aureus is reduced by nearly a factor of 30 compared to silanized SiO2surfaces. Therefore, hydrophobin coatings are of great interest for further use in the field of biomedical surface coating.

UR - https://www.scopus.com/pages/publications/105014889820

U2 - 10.1021/acsomega.4c11010

DO - 10.1021/acsomega.4c11010

M3 - Article

AN - SCOPUS:105014889820

SN - 2470-1343

VL - 10

SP - 38376

EP - 38384

JO - ACS Omega

JF - ACS Omega

IS - 34

ER -

Staphylococcus aureus Adhesion on Hydrophobin Coatings: Adhesion Forces and the Influence of Surface Charge

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