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不同临床材料上生物膜及生物膜基质蛋白的结构与功能动态变化

Structural and Functional Dynamics of Biofilms and Biofilm Matrix Proteins on Different Clinical Materials.

作者信息

Hiltunen Anna K, Savijoki Kirsi, Nyman Tuula A, Miettinen Ilkka, Ihalainen Petri, Peltonen Jouko, Fallarero Adyary

机构信息

Pharmaceutical Design and Discovery (PharmDD) Group, Pharmaceutical Biology, Division of Pharmaceutical Biosciences, Faculty of Pharmacy, University of Helsinki, Viikinkaari 5, 00014 Helsinki, Finland.

Department of Immunology, Institute of Clinical Medicine, University of Oslo and Rikshospitalet Oslo, 0372 Oslo, Norway.

出版信息

Microorganisms. 2019 Nov 20;7(12):584. doi: 10.3390/microorganisms7120584.

Abstract

Medical device-associated staphylococcal infections are a common and challenging problem. However, detailed knowledge of staphylococcal biofilm dynamics on clinically relevant surfaces is still limited. In the present study, biofilm formation of the ATCC 25923 strain was studied on clinically relevant materials-borosilicate glass, plexiglass, hydroxyapatite, titanium and polystyrene-at 18, 42 and 66 h. Materials with the highest surface roughness and porosity (hydroxyapatite and plexiglass) did not promote biofilm formation as efficiently as some other selected materials. Matrix-associated poly--acetyl-β-(1-6)-glucosamine (PNAG) was considered important in young (18 h) biofilms, whereas proteins appeared to play a more important role at later stages of biofilm development. A total of 460 proteins were identified from biofilm matrices formed on the indicated materials and time points-from which, 66 proteins were proposed to form the core surfaceome. At 18 h, the appearance of several r-proteins and glycolytic adhesive moonlighters, possibly via an autolysin (AtlA)-mediated release, was demonstrated in all materials, whereas classical surface adhesins, resistance- and virulence-associated proteins displayed greater variation in their abundances depending on the used material. Hydroxyapatite-associated biofilms were more susceptible to antibiotics than biofilms formed on titanium, but no clear correlation between the tolerance and biofilm age was observed. Thus, other factors, possibly the adhesive moonlighters, could have contributed to the observed chemotolerant phenotype. In addition, a protein-dependent matrix network was observed to be already well-established at the 18 h time point. To the best of our knowledge, this is among the first studies shedding light into matrix-associated surfaceomes of S. aureus biofilms grown on different clinically relevant materials and at different time points.

摘要

与医疗设备相关的葡萄球菌感染是一个常见且具有挑战性的问题。然而,对于葡萄球菌在临床相关表面上的生物膜动力学的详细了解仍然有限。在本研究中,研究了ATCC 25923菌株在临床相关材料——硼硅酸盐玻璃、有机玻璃、羟基磷灰石、钛和聚苯乙烯——上在18、42和66小时时的生物膜形成情况。表面粗糙度和孔隙率最高的材料(羟基磷灰石和有机玻璃)促进生物膜形成的效率不如其他一些选定材料。与基质相关的聚-N-乙酰-β-(1-6)-葡糖胺(PNAG)在年轻(18小时)生物膜中被认为很重要,而蛋白质似乎在生物膜发育的后期阶段发挥更重要的作用。从在指定材料和时间点形成的生物膜基质中总共鉴定出460种蛋白质,其中66种蛋白质被认为构成核心表面组。在18小时时,在所有材料中都证明了几种r蛋白和糖酵解黏附兼性蛋白可能通过自溶素(AtlA)介导的释放出现,而经典表面黏附素、抗性和毒力相关蛋白的丰度根据所用材料显示出更大的差异。与羟基磷灰石相关的生物膜比在钛上形成的生物膜对抗生素更敏感,但未观察到耐受性与生物膜年龄之间的明确相关性。因此,其他因素,可能是黏附兼性蛋白,可能导致了观察到的化学耐受表型。此外,在18小时时间点观察到一个依赖蛋白质的基质网络已经建立得很好。据我们所知,这是首批揭示在不同临床相关材料上和不同时间点生长的金黄色葡萄球菌生物膜与基质相关的表面组的研究之一。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/29d5/6955704/e18d01a56c42/microorganisms-07-00584-g001.jpg

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