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  • Efficacy and safety of biofilm dispersal by glycoside hydrolases in wounds.

Efficacy and safety of biofilm dispersal by glycoside hydrolases in wounds.

Biofilm (2021-11-27)
Whitni K Redman, Garrett S Welch, Avery C Williams, Addyson J Damron, Willem O Northcut, Kendra P Rumbaugh
ABSTRACT

Novel anti-biofilm and dispersal agents are currently being investigated in an attempt to combat biofilm-associated wound infections. Glycoside hydrolases (GHs) are enzymes that hydrolyze the glycosidic bonds between sugars, such as those found within the exopolysaccharides of the biofilm matrix. Previous studies have shown that GHs can weaken the matrix, inducing bacterial dispersal, and improving antibiotic clearance. Yet, the number of GH enzymes that have been examined for potential therapeutic effects is limited. In this study, we screened sixteen GHs for their ability to disperse mono-microbial and polymicrobial biofilms grown in different environments. Six GHs, α-amylase (source: A. oryzae), alginate lyase (source: various algae), pectinase (source: Rhizopus sp.), amyloglucosidase (source: A. niger), inulinase (source: A. niger), and xylanase (source: A. oryzae), exhibited the highest dispersal efficacy in vitro. Two GHs, α-amylase (source: Bacillus sp.) and cellulase (source: A. niger), used in conjunction with meropenem demonstrated infection clearing ability in a mouse wound model. GHs were also effective in improving antibiotic clearance in diabetic mice. To examine their safety, we screened the GHs for toxicity in cell culture. Overall, there was an inverse relationship between enzyme exposure time and cellular toxicity, with twelve out of sixteen GHs demonstrating some level of toxicity in cell culture. However, only one GH exhibited harmful effects in mice. These results further support the ability of GHs to improve antibiotic clearance of biofilm-associated infections and help lay a foundation for establishing GHs as therapeutic agents for chronic wound infections.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
Amyloglucosidase from Rhizopus sp., ≥40,000 units/g solid
Sigma-Aldrich
α-Amylase from porcine pancreas, Type I-A, PMSF treated, saline suspension, 700-1400 units/mg protein (E1%/280)
Sigma-Aldrich
Pectinase from Rhizopus sp., powder, 400-800 units/g solid
Sigma-Aldrich
β-Amylase from barley, Type II-B, 20-80 units/mg protein (biuret)
Sigma-Aldrich
Xylanase, powder, ≥2500 units/g, recombinant, expressed in Aspergillus oryzae
Sigma-Aldrich
Pectinase from Aspergillus niger, powder, slightly beige, >1 U/mg
Sigma-Aldrich
Amyloglucosidase from Aspergillus niger, powder, white, ~120 U/mg
Sigma-Aldrich
Inulinase from Aspergillus niger, lyophilized, powder, brown-gray, ~25 U/mg
Sigma-Aldrich
Alginate Lyase, powder, ≥10,000 units/g solid
Sigma-Aldrich
α-Amylase from Aspergillus oryzae, ≥150 units/mg protein (biuret)