SYSTEMIC AND FREE LOCAL ANTIBIOTIC DELIVERY METHOD TO PREVENT IMPLANT-RELATED INFECTION

Mirick GM, Sabin A, Hansen G, et al. SYSTEMIC AND FREE LOCAL ANTIBIOTIC DELIVERY METHOD TO PREVENT IMPLANT-RELATED INFECTION. Orthop Procs. 2019;101-B(SUPP_12):58-58. doi:10.1302/1358-992X.2019.12.058

Mirick, G. M., et al. “SYSTEMIC AND FREE LOCAL ANTIBIOTIC DELIVERY METHOD TO PREVENT IMPLANT-RELATED INFECTION.” Orthopaedic Proceedings, vol. 101-B, no. SUPP_12, 2019, pp. 58-58., https://doi.org/10.1302/1358-992X.2019.12.058

Mirick, G. M., Sabin, A., Hansen, G., Lindgren, B., Aparicio, C., Carlson, C. S., Bue, M., Larsen, O., Schmidt, A. H., Kyle, R., Gustilo, R. B., Tsukayama, D., & Bechtold, J. E. (2019). SYSTEMIC AND FREE LOCAL ANTIBIOTIC DELIVERY METHOD TO PREVENT IMPLANT-RELATED INFECTION. Orthopaedic Proceedings, 101-B(SUPP_12), 58-58. https://doi.org/10.1302/1358-992X.2019.12.058

Mirick, G. M., Sabin, A., Hansen, G., Lindgren, B., Aparicio, C., Carlson, C. S. et al. (2019) “SYSTEMIC AND FREE LOCAL ANTIBIOTIC DELIVERY METHOD TO PREVENT IMPLANT-RELATED INFECTION.” Orthopaedic Proceedings, 101-B(SUPP_12), pp. 58-58. Available at: https://doi.org/10.1302/1358-992X.2019.12.058

Mirick, G. M., A. Sabin, G. Hansen, B. Lindgren, C. Aparicio, C. S. Carlson, M. Bue, et al. “SYSTEMIC AND FREE LOCAL ANTIBIOTIC DELIVERY METHOD TO PREVENT IMPLANT-RELATED INFECTION.” Orthopaedic Proceedings 101-B, no. SUPP_12 (2019): 58-58. https://doi.org/10.1302/1358-992X.2019.12.058

Mirick GM, Sabin A, Hansen G, Lindgren B, Aparicio C, Carlson CS, et al. SYSTEMIC AND FREE LOCAL ANTIBIOTIC DELIVERY METHOD TO PREVENT IMPLANT-RELATED INFECTION. Orthop Procs. 2019 Oct 1;101-B(SUPP_12):58-58. https://doi.org/10.1302/1358-992X.2019.12.058

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Abstract

Introduction

We studied free (= local powder) tobramycin and doxycycline, and controlled release (= local lipid bilayer) doxycycline formulations in a rat model representing a generic joint infection. We hypothesized that evidence of infection (quantitative colony forming units (CFU), qualitative SEM, histopathology) (1a) would be reduced with local vs. systemic antibiotic, (1b) any antibiotic would be superior to control (2) there would be a difference among antibiotics, and (3) antibiotic would not be detectable in serum at 4-week euthanasia.

Methods

Study groups included infected and non-infected (1) control, (2) systemic ceftriaxone (daily), (3) local tobramycin, (4) local doxycycline and (5) controlled release doxycycline. With IACUC approval, (10 rats/group; power =0.8), 50-μl, 10×4 CFU Staphylococcus aureus, slowly injecting into distal femoral medullary canal, reliably created joint infection. Antibiotic formulation was introduced locally into cavity and joint, pin was inserted, and tissues closed. After 4-weeks, serum, pin, bone and synovium were obtained. CFU/ml of bone and synovium were quantified using macrotiter method. SEM imaged biofilm on surface of pin, histopathology identified tissue response, liquid chromatography/mass spectrometry measured plasma antibiotic. Kruskal-Wallis one-way ANOVA compared groups.

Results

Groups receiving antibiotic reported lower CFU/ml in synovium compared with control (no treatment) group (1b), but there was no difference between systemic, free or controlled antibiotics (1a). Different results with different antibiotics were shown, with free tobramycin reducing CFU/ml to a greater extent than free doxycycline in the synovium (2) (p<0.05). Antibiotic in plasma was nondetectable all groups (3). SEM revealed some biofilm on pin in all groups. Limitations include inoculation method, single observation period, administration of only one bacterial and antibiotic dose, and not including pairing local and systemic antibiotic.

Conclusion

There was no difference in infection reduction nor detectable antibiotic in serum for any antibiotic formulation, but CFU's in synovium differed based on antibiotic formulation.

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