Modulation of the Substitution Pattern of 5-Aryl-2-Aminoimidazoles Allows Fine-Tuning of Their Antibiofilm Activity Spectrum and Toxicity | Zendy

Elien Peeters | Zendy; Geert Hooyberghs | Zendy; Stijn Robijns | Zendy; Kai Waldrant | Zendy; Ami De Weerdt | Zendy; Nicolas Delattin | Zendy; Veerle Liebens | Zendy; Soňa Kucharíková | Zendy; Hélène Tournu | Zendy; Natalie Verstraeten | Zendy; Barbara Dovgan | Zendy; Lenart Girandon | Zendy; Mirjam Fröhlich | Zendy; Katrijn De Brucker | Zendy; Patrick Van Dijck | Zendy; Jan Michiels | Zendy; Bruno P.A. Cammue | Zendy; Karin Thevissen | Zendy; Jozef Vanderleyden | Zendy; Erik V. Van der Eycken | Zendy; Hans Steenackers | Zendy

Open Access

Modulation of the Substitution Pattern of 5-Aryl-2-Aminoimidazoles Allows Fine-Tuning of Their Antibiofilm Activity Spectrum and Toxicity

Author(s) -

Elien Peeters,

Geert Hooyberghs,

Stijn Robijns,

Kai Waldrant,

Ami De Weerdt,

Nicolas Delattin,

Veerle Liebens,

Soňa Kucharíková,

Hélène Tournu,

Natalie Verstraeten,

Barbara Dovgan,

Lenart Girandon,

Mirjam Fröhlich,

Katrijn De Brucker,

Patrick Van Dijck,

Jan Michiels,

Bruno P.A. Cammue,

Karin Thevissen,

Jozef Vanderleyden,

Erik V. Van der Eycken,

Hans Steenackers

Publication year - 2016

Publication title -

antimicrobial agents and chemotherapy

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.07

H-Index - 259

eISSN - 1070-6283

pISSN - 0066-4804

DOI - 10.1128/aac.00035-16

Subject(s) - biofilm , bacteria , candida albicans , microbiology and biotechnology , chemistry , salmonella enterica , pseudomonas aeruginosa , corpus albicans , aryl , antimicrobial , gram positive bacteria , toxicity , biology , salmonella , organic chemistry , genetics , alkyl

We previously synthesized several series of compounds, based on the 5-aryl-2-aminoimidazole scaffold, that showed activity preventing the formation of Salmonella enterica serovar Typhimurium and Pseudomonas aeruginosa biofilms. Here, we further studied the activity spectrum of a number of the most active N1- and 2N-substituted 5-aryl-2-aminoimidazoles against a broad panel of biofilms formed by monospecies and mixed species of bacteria and fungi. An N1-substituted compound showed very strong activity against the biofilms formed by Gram-negative and Gram-positive bacteria and the fungus Candida albicans but was previously shown to be toxic against various eukaryotic cell lines. In contrast, 2N-substituted compounds were nontoxic and active against biofilms formed by Gram-negative bacteria and C. albicans but had reduced activity against biofilms formed by Gram-positive bacteria. In an attempt to develop nontoxic compounds with potent activity against biofilms formed by Gram-positive bacteria for application in antibiofilm coatings for medical implants, we synthesized novel compounds with substituents at both the N1 and 2N positions and tested these compounds for antibiofilm activity and toxicity. Interestingly, most of these N1-,2N-disubstituted 5-aryl-2-aminoimidazoles showed very strong activity against biofilms formed by Gram-positive bacteria and C. albicans in various setups with biofilms formed by monospecies and mixed species but lost activity against biofilms formed by Gram-negative bacteria. In light of application of these compounds as anti-infective coatings on orthopedic implants, toxicity against two bone cell lines and the functionality of these cells were tested. The N1-,2N-disubstituted 5-aryl-2-aminoimidazoles in general did not affect the viability of bone cells and even induced calcium deposition. This indicates that modulating the substitution pattern on positions N1 and 2N of the 5-aryl-2-aminoimidazole scaffold allows fine-tuning of both the antibiofilm activity spectrum and toxicity.

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