Microbial Warfare on Three Fronts: Mixed Biofilm of Aspergillus fumigatus and Staphylococcus aureus on Primary Cultures of Human Limbo-Corneal Fibroblasts.

Adrián Ramírez-Granillo,Néstor O. Pérez,Luis Antonio Bautista-Hernández,Alfredo Domínguez-López,Itzel Margarita Córdova-Alcántara,Aída Verónica Rodríguez-Tovar,Fátima Sofía Magaña-Guerrero,Víctor Manuel Bautista-De Lucío,María de los Angeles Martínez-Rivera

doi:10.3389/fcimb.2021.646054

Adrián Ramírez-Granillo, Néstor O. Pérez + Show 7 more

Open Access

https://doi.org/10.3389/fcimb.2021.646054

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Abstract

BackgroundCoinfections with fungi and bacteria in ocular pathologies are increasing at an alarming rate. Two of the main etiologic agents of infections on the corneal surface, such as Aspergillus fumigatus and Staphylococcus aureus, can form a biofilm. However, mixed fungal–bacterial biofilms are rarely reported in ocular infections. The implementation of cell cultures as a study model related to biofilm microbial keratitis will allow understanding the pathogenesis in the cornea. The cornea maintains a pathogen-free ocular surface in which human limbo-corneal fibroblast cells are part of its cell regeneration process. There are no reports of biofilm formation assays on limbo-corneal fibroblasts, as well as their behavior with a polymicrobial infection.ObjectiveTo determine the capacity of biofilm formation during this fungal–bacterial interaction on primary limbo-corneal fibroblast monolayers.ResultsThe biofilm on the limbo-corneal fibroblast culture was analyzed by assessing biomass production and determining metabolic activity. Furthermore, the mixed biofilm effect on this cell culture was observed with several microscopy techniques. The single and mixed biofilm was higher on the limbo-corneal fibroblast monolayer than on abiotic surfaces. The A. fumigatus biofilm on the human limbo-corneal fibroblast culture showed a considerable decrease compared to the S. aureus biofilm on the limbo-corneal fibroblast monolayer. Moreover, the mixed biofilm had a lower density than that of the single biofilm. Antibiosis between A. fumigatus and S. aureus persisted during the challenge to limbo-corneal fibroblasts, but it seems that the fungus was more effectively inhibited.ConclusionThis is the first report of mixed fungal–bacterial biofilm production and morphological characterization on the limbo-corneal fibroblast monolayer. Three antibiosis behaviors were observed between fungi, bacteria, and limbo-corneal fibroblasts. The mycophagy effect over A. fumigatus by S. aureus was exacerbated on the limbo-corneal fibroblast monolayer. During fungal–bacterial interactions, it appears that limbo-corneal fibroblasts showed some phagocytic activity, demonstrating tripartite relationships during coinfection.

Highlights

Biofilms are microbial consortiums of sessile cells fused inside an extracellular matrix (ECM) that is composed of self-excreting biomolecules by the different microbial species
The phenotypic profile of the human limbo-corneal fibroblast cells (HLFCs) primary cultures was assessed by flow cytometry
Negative controls for each marker were included in the analysis, allowing the corroboration of the HLFC phenotype as VIM+cytokeratin antibody (CTK)-smooth muscle actin (SMA)- (Supplementary Figure S1)

Summary

Introduction

Biofilms are microbial consortiums of sessile cells fused inside an extracellular matrix (ECM) that is composed of self-excreting biomolecules by the different microbial species. Mixed fungal–bacterial biofilms (MFBBs) tend to be more prevalent than previously thought, especially in humans, and have been associated with antimicrobial resistance, postsurgical infections, and immunodeficiency diseases (Elder et al, 1996; Nucci and Marr, 2005; Wargo and Hogan, 2006; Jabra-Rizk, 2011; Peters et al, 2012; Diaz et al, 2014; Arvanitis and Mylonakis, 2015) These risk factors are determinants of the development of MFBB infections in the eye. The ocular surface is composed of the cornea, conjunctiva, and sclera; its main function is to protect the physical integrity of the eye (Busquet and Gabarel, 2008; Jiménez-Martıń ez et al, 2016; Lu and Liu, 2016) This protecting process depends on its ability to regenerate the epithelial layer under the influence of human limbo-corneal fibroblast cells (HLFCs). There are no reports of biofilm formation assays on limbo-corneal fibroblasts, as well as their behavior with a polymicrobial infection

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