Beyond Traditional Antimicrobials: A Model for Discovery of Novel Anti-infectives.

Front Microbiol

School of Biosciences and Biotechnology, Faculty of Science and Technology, Universiti Kebangsaan Malaysia Bangi, Malaysia.

Published: December 2016

The spread of antibiotic resistance amongst bacterial pathogens has led to an urgent need for new antimicrobial compounds with novel modes of action that minimize the potential for drug resistance. To date, the development of new antimicrobial drugs is still lagging far behind the rising demand, partly owing to the absence of an effective screening platform. Over the last decade, the nematode has been incorporated as a whole animal screening platform for antimicrobials. This development is taking advantage of the vast knowledge on worm physiology and how it interacts with bacterial and fungal pathogens. In addition to allowing for selection of compounds with promising anti-microbial properties, the whole animal screening system has also permitted the discovery of novel compounds targeting infection processes that only manifest during the course of pathogen infection of the host. Another advantage of using in the search for new antimicrobials is that the worm itself is a source of potential antimicrobial effectors which constitute part of its immune defense response to thwart infections. This has led to the evaluation of effector molecules, particularly antimicrobial proteins and peptides (APPs), as candidates for further development as therapeutic agents. In this review, we provide an overview on use of the model for identification of novel anti-infectives. We highlight some highly potential lead compounds obtained from -based screens, particularly those that target bacterial virulence or host defense to eradicate infections, a mechanism distinct from the action of conventional antibiotics. We also review the prospect of using APPs as an antimicrobial strategy to treat infections.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5133244PMC
http://dx.doi.org/10.3389/fmicb.2016.01956DOI Listing

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