Combination treatment with anti-RANKL and antibiotics for preventing joint destruction in septic arthritis
Zhicheng Hu, Meghshree Deshmukh, Anders Jarneborn, Miriam Bollmann, Carmen Corciulo, Pradeep Kumar Kopparapu, Abukar Ali, Mattias N. D. Svensson, Cecilia Engdahl, Rille Pullerits, Majd Mohammad, Tao Jin
Zhicheng Hu, Meghshree Deshmukh, Anders Jarneborn, Miriam Bollmann, Carmen Corciulo, Pradeep Kumar Kopparapu, Abukar Ali, Mattias N. D. Svensson, Cecilia Engdahl, Rille Pullerits, Majd Mohammad, Tao Jin
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Research Article Bone biology Infectious disease

Combination treatment with anti-RANKL and antibiotics for preventing joint destruction in septic arthritis

Abstract

Septic arthritis, the most severe joint disease, is frequently caused by Staphylococcus aureus (S. aureus). A substantial proportion of patients with septic arthritis experience poor joint outcomes, often necessitating joint replacement surgery. Here, we show that monocyte depletion confers full protection against bone erosion in a septic arthritis mouse model. In the infected synovium, Ly6Chi monocytes exhibited increased expression of osteoclastogenesis-related molecules, including CCR2, c-Fms, and RANK. S. aureus lipoproteins induced elevated levels of RANKL, MCSF, and CCL2 in joints, with synovial fibroblasts identified as the major RANKL producer. Anti-RANKL treatment prevented bone destruction in both local and hematogenous septic arthritis murine models. Importantly, combining anti-RANKL treatment with antibiotics provided robust protection against joint damage. Our results indicate that the infiltration and transformation of monocytes into bone-destructive, osteoclast-like cells are key mechanisms in septic arthritis. Combining anti-RANKL and antibiotic therapy represents a promising therapy against this devastating disease.

Authors

Zhicheng Hu, Meghshree Deshmukh, Anders Jarneborn, Miriam Bollmann, Carmen Corciulo, Pradeep Kumar Kopparapu, Abukar Ali, Mattias N. D. Svensson, Cecilia Engdahl, Rille Pullerits, Majd Mohammad, Tao Jin

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Figure 6

Combining antibiotics with anti-RANKL treatment proves superior to antibiotics alone in preventing joint damage in mice with septic arthritis.

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Combining antibiotics with anti-RANKL treatment proves superior to antib...
NMRI mice (n = 5/group) were intravenously injected with S. aureus Newman strain (5 × 106 CFU/mouse) and sacrificed on day 14 after infection. The following treatments were administered intraperitoneally twice daily commencing on day 5 after infection to the respective groups: isotype antibodies with PBS, anti-RANKL antibodies with PBS, isotype antibodies with cloxacillin, and anti-RANKL antibodies with cloxacillin. (A) The changes in body weight, (B) arthritis severities, (C) cumulative survival, (D) bacterial loads in the kidneys, (E) cumulative bone destruction scores, and (F) frequencies of bone destruction of the joints from all 4 limbs were assessed by μCT scan. Data are presented as mean with SEM. Statistical evaluations were performed using 2-way ANOVA with Tukey’s multiple-comparison test (A and B), log-rank (Mantel-Cox) test (C), 1-way ANOVA with Holm-Šídák multiple-comparison test (D), Kruskal-Wallis test with Dunn’s multiple-comparison test (E), or Fisher’s exact test (F). a, anti-RANKL + PBS vs. anti-RANKL + cloxacillin; b, anti-RANKL + PBS vs. isotype control + cloxacillin; c, anti-RANKL + cloxacillin vs. isotype control + PBS; d, isotype control + cloxacillin vs. isotype control + PBS. *P < 0.05; **P < 0.01; ***P < 0.001.