Determination of disc breakpoints and evaluation of Etests for tigecycline susceptibility testing by the BSAC method

doi:10.1093/jac/dkm297

JAC Advance Access originally published online on August 18, 2007
Journal of Antimicrobial Chemotherapy 2007 60(4):770-774; doi:10.1093/jac/dkm297

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© The Author 2007. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. All rights reserved. For Permissions, please e-mail: journals.permissions@oxfordjournals.org

Determination of disc breakpoints and evaluation of Etests for tigecycline susceptibility testing by the BSAC method

R. Hope^*, T. Parsons, S. Mushtaq, D. James and D. M. Livermore

Antibiotic Resistance and Monitoring Reference Laboratory, Centre for Infections, Health Protection Agency, 61 Colindale Avenue, London NW9 5EQ, UK

Received 25 April 2007; returned 12 July 2007; revised 7 June 2007; accepted 13 July 2007

^* Corresponding author. Tel: +44-20-8327-6493; Fax: +44-20-8327-6264; E-mail: russell.hope{at}hpa.org.uk

Background: Tigecycline has been recently licensed in Europe for intra-abdominaland complicated skin and soft tissue infections. We determinedzone breakpoints for use with 15 µg tigecycline discsand evaluated Etests for the routine determination of tigecyclinesusceptibility by BSAC methods.

Methods: Disc zones for 2236 isolates and MICs by Etest for 531 isolateswere compared with MICs obtained by the BSAC agar dilution method.

Results: Based on error minimization, we propose zone breakpoints for15 µg tigecycline discs as follows: ${alpha}$ /ß-haemolyticstreptococci, S $≥$ 25 mm, R $≤$ 19 mm; Acinetobacter spp. and Enterobacteriaceae,S $≥$ 24 mm, R $≤$ 19 mm; Enterococcus spp., S $≥$ 21 mm, R $≤$ 20 mm; Haemophilusspp., S $≥$ 28 mm, R $≤$ 27; Streptococcus pneumoniae, S $≥$ 24 mm, R $≤$ 23 mm; and staphylococci, S $≥$ 26 mm, R $≤$ 25 mm. These criteriagave overall false resistance rates of $≤$ 0.8% and false susceptibilityrates of $≤$ 0.7%. Tigecycline Etests, used on Iso-Sensitest agar,gave MICs within one doubling dilution of those by agar dilutionin 97% of cases. Categorization agreement was good for isolateswith borderline susceptibility or resistance—a group whereEtests are likely to be used in order to verify disc-based results.MICs for highly susceptible ${alpha}$ -haemolytic streptococci were underestimatedby Etest, but this seems unlikely to be significant.

Conclusions: Disc breakpoints corresponding to BSAC MIC breakpoints weredefined for 15 µg tigecycline discs and have been adoptedby the BSAC. Tigecycline Etest gave results in good agreementwith agar dilution.

Keywords: diagnostic tests , disc diffusion , MIC determination

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