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How quickly can we predict trimethoprim resistance using alchemical free energy methods?

Abstract:
The emergence of antimicrobial resistance threatens modern medicine and necessitates more personalized treatment of bacterial infections. Sequencing the whole genome of the pathogen(s) in a clinical sample offers one way to improve clinical microbiology diagnostic services, and has already been adopted for tuberculosis in some countries. A key weakness of a genetics clinical microbiology is it cannot return a result for rare or novel genetic variants and therefore predictive methods are required. Non-synonymous mutations in the S. aureusdfrB gene can be successfully classified as either conferring resistance (or not) by calculating their effect on the binding free energy of the antibiotic, trimethoprim. The underlying approach, alchemical free energy methods, requires large numbers of molecular dynamics simulations to be run. We show that a large number (N = 15) of binding free energies calculated from a series of very short (50 ps) molecular dynamics simulations are able to satisfactorily classify all seven mutations in our clinically derived testset. A result for a single mutation could therefore be returned in less than an hour, thereby demonstrating that this or similar methods are now sufficiently fast and reproducible for clinical use.
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.1098/rsfs.2019.0141

Authors


More by this author
Institution:
University of Oxford
Division:
MSD
Department:
NDM
Sub department:
NDM Experimental Medicine
Role:
Author


Publisher:
The Royal Society
Journal:
Interface Focus More from this journal
Volume:
10
Issue:
6
Article number:
20190141
Publication date:
2020-10-16
Acceptance date:
2020-09-11
DOI:
EISSN:
2042-8901


Language:
English
Keywords:
Pubs id:
1138221
Local pid:
pubs:1138221
Deposit date:
2020-10-19

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