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疏水蛋白涂层上的粘附:粘附力及表面电荷的影响

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

作者信息

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

机构信息

Experimental Physics, Center for Biophysics, Saarland University, Saarbrücken 66123, Germany.

Department of Electrical Engineering, Trier University of Applied Science, Trier 54293, Germany.

出版信息

ACS Omega. 2025 Aug 20;10(34):38376-38384. doi: 10.1021/acsomega.4c11010. eCollection 2025 Sep 2.

Abstract

() 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 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 strain SA113 on naive and protein-coated silicon surfaces (SiO). In addition to the wild type, we used the SA113 Δ 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 SiO surfaces 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 strain binds to hydrophobin-coated surfaces, we show that the adhesion of 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 is reduced by nearly a factor of 30 compared to silanized SiO surfaces. Therefore, hydrophobin coatings are of great interest for further use in the field of biomedical surface coating.

摘要

(某细菌物种)是能够在植入物上形成多层生物膜的细菌种类之一。在植入式医疗设备上形成的此类生物膜通常需要移除植入物,以避免败血症,在最坏的情况下,甚至会导致患者死亡。为了解决不需要的生物膜形成问题,必须了解并防止其第一步,即粘附。因此,开发用于植入材料的降低粘附力的表面涂层至关重要。在这项工作中,我们使用单细胞力谱分析生物膜形成菌株SA113在原始和蛋白质包被的硅表面(SiO)上的粘附情况。除了野生型,我们还使用SA113 Δ敲除突变体进一步研究细胞壁脂磷壁酸的d - 丙氨酰化的影响。为了研究表面电荷如何影响粘附,我们用两亲性II类疏水蛋白包被硅烷化的SiO表面。使用了天然存在的疏水蛋白HFBI以及HFBI变体D40Q/D43N,由于两个酸性天冬氨酸残基的交换,该变体在生理pH下带负电荷较少。这两种类型的疏水蛋白包被表面在粗糙度和润湿性方面彼此相似,但仅在电荷方面有所不同。通过测量每个菌株与疏水蛋白包被表面结合的力,我们表明在表面的粘附可以受到目标表面暴露的电荷的影响。因此,除了氢键之外,细胞与亲水性表面之间的静电相互作用也控制着在这些表面上的粘附。此外,我们发现对于两种HFBI涂层,与硅烷化的SiO表面相比,SA113的粘附强度降低了近30倍。因此,疏水蛋白涂层在生物医学表面涂层领域的进一步应用中具有很大的吸引力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4e14/12409555/e2e460de0240/ao4c11010_0001.jpg

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