EFFECTS OF LOW DOSE BMP-2 AND IMMUNOMODULATION TARGETING IL-1ß ON FRACTURE HEALING IN A FEMUR DEFECT MODEL IN RATS

Schröder M, Gens L, Arens D, et al. EFFECTS OF LOW DOSE BMP-2 AND IMMUNOMODULATION TARGETING IL-1ß ON FRACTURE HEALING IN A FEMUR DEFECT MODEL IN RATS. Orthop Procs. 2024;106-B(SUPP_18):30-30. doi:10.1302/1358-992X.2024.18.030

Schröder, M., et al. “EFFECTS OF LOW DOSE BMP-2 AND IMMUNOMODULATION TARGETING IL-1ß ON FRACTURE HEALING IN A FEMUR DEFECT MODEL IN RATS.” Orthopaedic Proceedings, vol. 106-B, no. SUPP_18, 2024, pp. 30-30., https://doi.org/10.1302/1358-992X.2024.18.030

Schröder, M., Gens, L., Arens, D., Giger, N., Gehweiler, D., Nehrbass, D., Zderic, I., Zeiter, S., Stoddart, M., & Wehrle, E. (2024). EFFECTS OF LOW DOSE BMP-2 AND IMMUNOMODULATION TARGETING IL-1ß ON FRACTURE HEALING IN A FEMUR DEFECT MODEL IN RATS. Orthopaedic Proceedings, 106-B(SUPP_18), 30-30. https://doi.org/10.1302/1358-992X.2024.18.030

Schröder, M., Gens, L., Arens, D., Giger, N., Gehweiler, D., Nehrbass, D. et al. (2024) “EFFECTS OF LOW DOSE BMP-2 AND IMMUNOMODULATION TARGETING IL-1ß ON FRACTURE HEALING IN A FEMUR DEFECT MODEL IN RATS.” Orthopaedic Proceedings, 106-B(SUPP_18), pp. 30-30. Available at: https://doi.org/10.1302/1358-992X.2024.18.030

Schröder, M., L. Gens, D. Arens, N. Giger, D. Gehweiler, D. Nehrbass, I. Zderic, S. Zeiter, M. Stoddart, and E. Wehrle. “EFFECTS OF LOW DOSE BMP-2 AND IMMUNOMODULATION TARGETING IL-1ß ON FRACTURE HEALING IN A FEMUR DEFECT MODEL IN RATS.” Orthopaedic Proceedings 106-B, no. SUPP_18 (2024): 30-30. https://doi.org/10.1302/1358-992X.2024.18.030

Schröder M, Gens L, Arens D, Giger N, Gehweiler D, Nehrbass D, et al. EFFECTS OF LOW DOSE BMP-2 AND IMMUNOMODULATION TARGETING IL-1ß ON FRACTURE HEALING IN A FEMUR DEFECT MODEL IN RATS. Orthop Procs. 2024 Nov 14;106-B(SUPP_18):30-30. https://doi.org/10.1302/1358-992X.2024.18.030

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Abstract

Introduction

Immunomodulation represents a novel strategy to improve bone healing in combination with low doses of bone morphogenetic growth factors like BMP-2. This study aims to investigate the effect and timing of monoclonal anti-IL-1ß antibody administration with 1μg BMP-2 on bone healing over 14 weeks in a rat femur segmental defect model.

Method

2 mm femoral defects were created in 22-27 weeks-old female Fischer F344 rats, internally fixed with a plate (animal license: GR/19/2022) using established protocols for analgesia and anesthesia. Animals (n=4/group) received either a collagen sponge, a collagen sponge+1μg BMP-2 (InductOs, Medtronic) or a collagen sponge+1μg BMP-2 with a monoclonal anti-IL-1ß antibody (BioXCell, 10 mg/ml), administered intravenously under anesthesia every third day until day 15, from day 0 or 3. In vivo micro-CT was performed after surgery and at 2, 3, 4, 6, 8, 10 and 14-weeks post-OP. Mechanical properties of the operated femurs were assessed by 4-point bending (Instron5866) and compared to contralateral femurs (one-way ANOVA, GraphPad Prism8). Histopathological analysis was performed semi-quantitatively on Giemsa-Eosin-stained sections (Olympus BX63) using a six-grade severity grading scale.

Result

Operated femurs with BMP-2 reached an average stiffness of 91±37% of contralateral femurs, femurs in IL-1ß groups 105±11% (day 0) and 111±12% (day 3). Administration of anti-IL-1ß+1μg BMP-2 led to faster cortical bridging (3/4 femurs bridged by week 4 for day 0, 4/4 for day 3) than 1μg BMP-2 alone (0/4 by week 4). Micro-CT results confirmed histopathological evaluation, as collagen sponge alone led to non-union, complete bicortical bridging was observed for 3/4 femurs in the BMP-2 group and for 4/4 femurs in the IL-1β groups after 14 weeks.