STRUGGLING WITH A CEFAZOLIN IMPREGNATION PROTOCOL OF BONE CHIPS: THE EFFECT OF THE TIMING OF THE IMPREGNATION AND GAMMA IRRADIATION ON THE CEFAZOLIN RELEASE

Karen Dendoncker; Guy Putzeys; Olivier Cornu; Tara Nieuwenhuizen; Manon Bertrand; Henriëtte Valster; Kathleen Croes

doi:10.1302/1358-992X.2023.17.045

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General Orthopaedics

STRUGGLING WITH A CEFAZOLIN IMPREGNATION PROTOCOL OF BONE CHIPS: THE EFFECT OF THE TIMING OF THE IMPREGNATION AND GAMMA IRRADIATION ON THE CEFAZOLIN RELEASE

The European Bone and Joint Infection Society (EBJIS) Meeting, Basel, Switzerland, 12–14 October 2023.

Karen Dendoncker
Guy Putzeys
Olivier Cornu
Tara Nieuwenhuizen
Manon Bertrand
Henriëtte Valster
Kathleen Croes

STRUGGLING WITH A CEFAZOLIN IMPREGNATION PROTOCOL OF BONE CHIPS: THE EFFECT OF THE TIMING OF THE IMPREGNATION AND GAMMA IRRADIATION ON THE CEFAZOLIN RELEASE

Dendoncker K, Putzeys G, Cornu O, et al. STRUGGLING WITH A CEFAZOLIN IMPREGNATION PROTOCOL OF BONE CHIPS: THE EFFECT OF THE TIMING OF THE IMPREGNATION AND GAMMA IRRADIATION ON THE CEFAZOLIN RELEASE. Orthop Procs. 2023;105-B(SUPP_17):45-45. doi:10.1302/1358-992X.2023.17.045

Dendoncker, Karen, et al. “STRUGGLING WITH A CEFAZOLIN IMPREGNATION PROTOCOL OF BONE CHIPS: THE EFFECT OF THE TIMING OF THE IMPREGNATION AND GAMMA IRRADIATION ON THE CEFAZOLIN RELEASE.” Orthopaedic Proceedings, vol. 105-B, no. SUPP_17, 2023, pp. 45-45., https://doi.org/10.1302/1358-992X.2023.17.045

Dendoncker, K., Putzeys, G., Cornu, O., Nieuwenhuizen, T., Bertrand, M., Valster, H., & Croes, K. (2023). STRUGGLING WITH A CEFAZOLIN IMPREGNATION PROTOCOL OF BONE CHIPS: THE EFFECT OF THE TIMING OF THE IMPREGNATION AND GAMMA IRRADIATION ON THE CEFAZOLIN RELEASE. Orthopaedic Proceedings, 105-B(SUPP_17), 45-45. https://doi.org/10.1302/1358-992X.2023.17.045

Dendoncker, K., Putzeys, G., Cornu, O., Nieuwenhuizen, T., Bertrand, M., Valster, H. et al. (2023) “STRUGGLING WITH A CEFAZOLIN IMPREGNATION PROTOCOL OF BONE CHIPS: THE EFFECT OF THE TIMING OF THE IMPREGNATION AND GAMMA IRRADIATION ON THE CEFAZOLIN RELEASE.” Orthopaedic Proceedings, 105-B(SUPP_17), pp. 45-45. Available at: https://doi.org/10.1302/1358-992X.2023.17.045

Dendoncker, Karen, Guy Putzeys, Olivier Cornu, Tara Nieuwenhuizen, Manon Bertrand, Henriëtte Valster, and Kathleen Croes. “STRUGGLING WITH A CEFAZOLIN IMPREGNATION PROTOCOL OF BONE CHIPS: THE EFFECT OF THE TIMING OF THE IMPREGNATION AND GAMMA IRRADIATION ON THE CEFAZOLIN RELEASE.” Orthopaedic Proceedings 105-B, no. SUPP_17 (2023): 45-45. https://doi.org/10.1302/1358-992X.2023.17.045

Dendoncker K, Putzeys G, Cornu O, Nieuwenhuizen T, Bertrand M, Valster H, et al. STRUGGLING WITH A CEFAZOLIN IMPREGNATION PROTOCOL OF BONE CHIPS: THE EFFECT OF THE TIMING OF THE IMPREGNATION AND GAMMA IRRADIATION ON THE CEFAZOLIN RELEASE. Orthop Procs. 2023 Nov 24;105-B(SUPP_17):45-45. https://doi.org/10.1302/1358-992X.2023.17.045

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Abstract

Aim

Local antibiotics released through a carrier is a commonly used technique to prevent infection in orthopaedic procedures. An interesting carrier in aseptic bone reconstructive surgery are bone chips impregnated with AB solution. Systemically administered Cefazolin (CFZ) is used for surgical site infection prophylaxis however in vitro study showed that fresh frozen and processed bone chips impregnated with CFZ solution completely release the CFZ within a few hours. On the other hand irradiated freeze-dried bone chips, treated with supercritical CO2 (scCO2) have been shown to be an efficient carrier for the antibiotics vancomycine or tobramycine.

With this pilot study we wanted to investigate if CFZ solution impregnation of bone chips treated with scCO2 shows a more favorable release pattern of CFZ.

Method

The bone chips were prepared using the standard scCO2 protocol and were impregnated with 100 mg/ml cefazolin at different timepoints during the process: before freeze drying (BC type A), after freeze drying (BC type B) and after gamma-irradiation. 0.5g of the impregnated bone grafts were incubated with 5ml of fetal calf serum (FCS) at 37°C. At 2, 4, 6, 8 and 24h of incubation 200µl of eluate was taken for analysis. After 24h the remaining FCS was removed, bone grafts were washed and new FCS (5ml) was added. Consecutive eluate samples were taken at 48, 72 and 96h of incubation.

The concentration of CFZ in the eluates was measured with the validated UPLC-DAD method. Analysis was performed in triplicate.

Results

The mean concentration of CFZ in the eluate obtained from BC type A incubated for 2h was higher compared to BC type B, respectively 581 mg/l and 297 mg/l. However, the elution profile is the same for both types: the CFZ concentration in the eluates drops within the first 24h from 581 mg/l to 365 mg/l (37%) for BC type A and from 297 mg/l to 132 mg/l (56%) for BC type B. After 24h no further significant CFZ release is seen.

Impregnation of the bone chips before or after gamma irradiation did not affect this elution profile.

Conclusions

Bone chips treated with scCO2 show a comparable elution pattern compared to non-scCO2 treated bone chips. AB release depends on the properties of the AB, making it impossible to copy the same impregnation protocol for different antibiotics. The stability of CFZ in solution at 37°C and its release are a major concern when establishing an impregnation protocol with CFZ.

Email: guy.putzeys@azgroeninge.be