IS DÉLAFLOXACINE A THERAPEUTIC OPTION FOR BONE AND JOINT INFECTIONS? A CRIOGO MULTICENTRE RETROSPECTIVE STUDY

Tessier E, d'Epenoux Louise R, Lartigue M, et al. IS DÉLAFLOXACINE A THERAPEUTIC OPTION FOR BONE AND JOINT INFECTIONS? A CRIOGO MULTICENTRE RETROSPECTIVE STUDY. Orthop Procs. 2023;105-B(SUPP_17):42-42. doi:10.1302/1358-992X.2023.17.042

Tessier, Eve, et al. “IS DÉLAFLOXACINE A THERAPEUTIC OPTION FOR BONE AND JOINT INFECTIONS? A CRIOGO MULTICENTRE RETROSPECTIVE STUDY.” Orthopaedic Proceedings, vol. 105-B, no. SUPP_17, 2023, pp. 42-42., https://doi.org/10.1302/1358-992X.2023.17.042

Tessier, E., d'Epenoux Louise, R., Lartigue, M., Guerin, F., Plouzeau-Jayle, C., Tandé, D., Chenouard, R., Bemer, P., & Corvec, S. (2023). IS DÉLAFLOXACINE A THERAPEUTIC OPTION FOR BONE AND JOINT INFECTIONS? A CRIOGO MULTICENTRE RETROSPECTIVE STUDY. Orthopaedic Proceedings, 105-B(SUPP_17), 42-42. https://doi.org/10.1302/1358-992X.2023.17.042

Tessier, E., d'Epenoux Louise, R., Lartigue, M., Guerin, F., Plouzeau-Jayle, C., Tandé, D. et al. (2023) “IS DÉLAFLOXACINE A THERAPEUTIC OPTION FOR BONE AND JOINT INFECTIONS? A CRIOGO MULTICENTRE RETROSPECTIVE STUDY.” Orthopaedic Proceedings, 105-B(SUPP_17), pp. 42-42. Available at: https://doi.org/10.1302/1358-992X.2023.17.042

Tessier, Eve, Ruffier d'Epenoux Louise, Marie-Frédérique Lartigue, François Guerin, Chloé Plouzeau-Jayle, Didier Tandé, Rachel Chenouard, Pascale Bemer, and Stephane Corvec. “IS DÉLAFLOXACINE A THERAPEUTIC OPTION FOR BONE AND JOINT INFECTIONS? A CRIOGO MULTICENTRE RETROSPECTIVE STUDY.” Orthopaedic Proceedings 105-B, no. SUPP_17 (2023): 42-42. https://doi.org/10.1302/1358-992X.2023.17.042

Tessier E, d'Epenoux Louise R, Lartigue M, Guerin F, Plouzeau-Jayle C, Tandé D, et al. IS DÉLAFLOXACINE A THERAPEUTIC OPTION FOR BONE AND JOINT INFECTIONS? A CRIOGO MULTICENTRE RETROSPECTIVE STUDY. Orthop Procs. 2023 Nov 24;105-B(SUPP_17):42-42. https://doi.org/10.1302/1358-992X.2023.17.042

Copy to clipboard

BibTeX

EndNote

RIS

Abstract

Abstract Background

The treatment of bone and joint infections (BJI) involving multi-drug resistant bacteria remains a challenge. MDR Staphylococcus epidermidis (MDRSE) clones, resistant to methicillin, clindamycin, levofloxacin, rifampicin and even linezolid, have been reported worldwide. The interest of delafloxacin (DFX), theoretically active on MRSA, remains to be evaluated with respect to MDRSE.

Purpose

Our objective was to evaluate during a retrospective multicenter study the DFX minimal inhibitory concentrations (MICs) and compare its efficacy between ofloxacin-susceptible and ofloxacin-resistant S. epidermidis clinical strains involved in BJI.

Methods

In this multicenter retrospective study (Reference centers from the West part of France, CRIOGO), 529 strains were collected mostly from BJI. DFX MICs were determined by using a 0.5 Mc Farland bacterial inoculum on Mueller-Hinton agar plates with gradient strips incubated for 24h at 35°C. For S. aureus, breakpoints differentiate skin and soft tissue infections from other infections. Breakpoints followed 2022 EUCAST criteria, with S. aureus values adopted for S. epidermidis.

Results

Of the 529 strains collected, 355 were from prosthetic infections, 159 from synthetic infections and 15 from non-device infections. 152 strains were susceptible to ofloxacin (110 males vs 42 females) and 377 resistant (210 vs 167). As presented in Figure 1, all the ofloxacin-susceptible strains presented a DFX MIC ≤0.006mg/L. Resistant strains presented a double population distribution, with 3.7% categorized susceptible according to skin and soft tissues infections breakpoint, against 88.9% according to other breakpoint infections (0.016 or 0.25mg/L respectively).

Conclusion

DFX shows excellent activity against ofloxacine-susceptible strains. Concerning the ofloxacin-resistant strains, more than 80% strains or less than 10% can be considered as DFX-susceptible depending on the breakpoints used. Further clinical studies are needed to validate the real breakpoints that must be used in MDRSE BJI, allowing a microbiological cure and a favourable clinical outcome.

For any tables or figures, please contact the authors directly.

Email: stephane.corvec@chu-nantes.fr