Abstract

Biofilm is a complex structure formed as a result of the accumulation of bacterial cell clusters on a surface, surrounded by extracellular polysaccharide substances (EPSs). Biofilm-related bacterial infections are a significant challenge for clinical treatment. Therefore, the main goal of our study was to design a complementary approach in biofilm characterization before and after the antibiotic treatment. The 16S rRNA gene sequencing allowed for the identification of Bacillus tequilensis, as a microbial model of the biofilm formation. Capillary electrophoresis demonstrates the capability to characterize and show the differences of the electrophoretic mobility between biofilms untreated and treated with antibiotics: amoxicillin, gentamicin and metronidazole. Electrophoretic results show the clumping phenomenon (amoxicillin and gentamicin) as a result of a significant change on the surface electric charge of the cells. The stability of the dispersion study, the molecular profile analysis, the viability of bacterial cells and the scanning morphology imaging were also investigated. The microscopic and spectrometry study pointed out the degradation/remodeling of the EPSs matrix, the inhibition of the cell wall synthesis and blocking the ribosomal protein synthesis by amoxicillin and gentamicin. However, untreated and treated bacterial cells show a high stability for the biofilm formation system. Moreover, on the basis of the type of the antibiotic treatment, the mechanism of used antibiotics in cell clumping and degradation were proposed.

Highlights

  • Publisher’s Note: MDPI stays neutralThe bacterial infections associated with biofilm constitute a serious problem in the clinical area [1,2]

  • The proposed scheme is concerned with the mechanism of studied antibiotics on the phenomenon of clumping and degradation in the bacterial cell of B. tequilensis

  • The proposed scheme is concerned with the mechanism of studied antibiotics on the phenomenon of is clumping and degradation in the bacterial cell of B

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Summary

Introduction

The bacterial infections associated with biofilm constitute a serious problem in the clinical area [1,2]. Biofilm impairs human defense mechanisms and creates a platform for microorganisms to use a range of strategies to control antibiotics resistance, including spore cell production, the multilayer system of bacteria cells and antimicrobial resistance [3,4]. The increase in polysaccharide components in the matrix results in more free functional groups able to interact with other bacterial cells or active molecules such as antibiotics. It determines a significant resistance of the microorganisms in biofilm [7,8,9,10,11]

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