PROLONGED CEFAZOLIN RELEASE FROM HYDROGEL-IMPREGNATED BONE CHIPS

C. Duportail; M. Gerard; C. Kathleen; G. Putzeys; L. Thorrez

doi:10.1302/1358-992X.2019.14.019

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General Orthopaedics

PROLONGED CEFAZOLIN RELEASE FROM HYDROGEL-IMPREGNATED BONE CHIPS

European Bone and Joint Infection Society (EBJIS) meeting, Antwerp, Belgium, September 2019.

C. Duportail
M. Gerard
C. Kathleen
G. Putzeys
L. Thorrez

PROLONGED CEFAZOLIN RELEASE FROM HYDROGEL-IMPREGNATED BONE CHIPS

Duportail C, Gerard M, Kathleen C, Putzeys G, Thorrez L. PROLONGED CEFAZOLIN RELEASE FROM HYDROGEL-IMPREGNATED BONE CHIPS. Orthop Procs. 2019;101-B(SUPP_14):19-19. doi:10.1302/1358-992X.2019.14.019

Duportail, C., et al. “PROLONGED CEFAZOLIN RELEASE FROM HYDROGEL-IMPREGNATED BONE CHIPS.” Orthopaedic Proceedings, vol. 101-B, no. SUPP_14, 2019, pp. 19-19., https://doi.org/10.1302/1358-992X.2019.14.019

Duportail, C., Gerard, M., Kathleen, C., Putzeys, G., & Thorrez, L. (2019). PROLONGED CEFAZOLIN RELEASE FROM HYDROGEL-IMPREGNATED BONE CHIPS. Orthopaedic Proceedings, 101-B(SUPP_14), 19-19. https://doi.org/10.1302/1358-992X.2019.14.019

Duportail, C., Gerard, M., Kathleen, C., Putzeys, G. and Thorrez, L. (2019) “PROLONGED CEFAZOLIN RELEASE FROM HYDROGEL-IMPREGNATED BONE CHIPS.” Orthopaedic Proceedings, 101-B(SUPP_14), pp. 19-19. Available at: https://doi.org/10.1302/1358-992X.2019.14.019

Duportail, C., M. Gerard, C. Kathleen, G. Putzeys, and L. Thorrez. “PROLONGED CEFAZOLIN RELEASE FROM HYDROGEL-IMPREGNATED BONE CHIPS.” Orthopaedic Proceedings 101-B, no. SUPP_14 (2019): 19-19. https://doi.org/10.1302/1358-992X.2019.14.019

Duportail C, Gerard M, Kathleen C, Putzeys G, Thorrez L. PROLONGED CEFAZOLIN RELEASE FROM HYDROGEL-IMPREGNATED BONE CHIPS. Orthop Procs. 2019 Dec 1;101-B(SUPP_14):19-19. https://doi.org/10.1302/1358-992X.2019.14.019

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Abstract

Aim

Allograft bone chips used in complex bone reconstruction procedures are associated with an increased infection risk. The perioperative use of systemic cefazolin is standard to prevent infection, but is less effective in the presence of avascular bone grafts. Bone chips have been described as a carrier for local delivery of antibiotics, but impregnation with cefazolin in a prophylactic setting has not been described. We aimed to obtain a prolonged cefazolin release from bone chips to maximize the prophylactic effect.

Method

Three types of bone chips were evaluated: fresh frozen, decellularized frozen and decellularized lyophilized. Bone chips were incubated with 20 mg/ml cefazolin or treated with liquid hydrogel containing either 1 mg/ml fibrin or 1 mg/ml collagen and 20 mg/ml cefazolin. The cefazolin hydrogel was distributed in the porous structure by short vacuum treatment. Bone chips with cefazolin but without hydrogel were incubated for 20 min- 4h under atmospheric pressure or under vacuum. Cefazolin elution of bone chips was carried out in fetal bovine serum and analyzed by Ultra Performance Liquid Chromatography – Diode Array Detection.

Results

Without hydrogel, cefazolin release was limited to 4 hours. When vacuum was applied during impregnation, elution of cefazolin exceeding the MIC (minimal inhibitory concentration) from decellularized lyophilized bone chips was obtained for 36 hours. Use of a collagen hydrogel and vacuum treatment resulted in a high concentration at 24 hours, but did not support prolonged release for any of the three types of tested bone chips. In contrast, combination of decellularized frozen bone chips with fibrin hydrogel resulted in an initial release of 533 μg/ml, declining to the MIC at 72 hours, while no longer measurable after 92 hours. Such elution profile is desirable, since high initial levels are important to maximize antibacterial action whereas the complete wash out prevents antibiotic resistance. By increasing the cefazolin concentration during impregnation, elution above the MIC could be obtained for 120 hours. Impregnated bone chips stored at −20° C for 3 months performed similarly to freshly impregnated bone chips.