3.O.09 VIVO AND IN VITRO EFFECTS OF BISPHOSPHONATE TREATMENT ON GIANT CELL TUMOUR OF BONE

Gibbons C, Jones F, Taylor R, et al. 3.O.09 VIVO AND IN VITRO EFFECTS OF BISPHOSPHONATE TREATMENT ON GIANT CELL TUMOUR OF BONE. Orthop Procs. 2010;92-B(SUPP_III):440-440. doi:10.1302/0301-620X.92BSUPP_III.0920440c

Gibbons, CLMH, et al. “3.O.09 VIVO AND IN VITRO EFFECTS OF BISPHOSPHONATE TREATMENT ON GIANT CELL TUMOUR OF BONE.” Orthopaedic Proceedings, vol. 92-B, no. SUPP_III, 2010, pp. 440-440., https://doi.org/10.1302/0301-620X.92BSUPP_III.0920440c

Gibbons, C., Jones, F., Taylor, R., Knowles, H., Hogendoorn, P., Wass, J., Balke3, M., Gebert3, C., & Athanasou, N. A. (2010). 3.O.09 VIVO AND IN VITRO EFFECTS OF BISPHOSPHONATE TREATMENT ON GIANT CELL TUMOUR OF BONE. Orthopaedic Proceedings, 92-B(SUPP_III), 440-440. https://doi.org/10.1302/0301-620X.92BSUPP_III.0920440c

Gibbons, C., Jones, F., Taylor, R., Knowles, H., Hogendoorn, P., Wass, J. et al. (2010) “3.O.09 VIVO AND IN VITRO EFFECTS OF BISPHOSPHONATE TREATMENT ON GIANT CELL TUMOUR OF BONE.” Orthopaedic Proceedings, 92-B(SUPP_III), pp. 440-440. Available at: https://doi.org/10.1302/0301-620X.92BSUPP_III.0920440c

Gibbons, CLMH, F. Jones, R. Taylor, H. Knowles, P Hogendoorn, JAH Wass, M Balke3, C Gebert3, and N A Athanasou. “3.O.09 VIVO AND IN VITRO EFFECTS OF BISPHOSPHONATE TREATMENT ON GIANT CELL TUMOUR OF BONE.” Orthopaedic Proceedings 92-B, no. SUPP_III (2010): 440-440. https://doi.org/10.1302/0301-620X.92BSUPP_III.0920440c

Gibbons C, Jones F, Taylor R, Knowles H, Hogendoorn P, Wass J, et al. 3.O.09 VIVO AND IN VITRO EFFECTS OF BISPHOSPHONATE TREATMENT ON GIANT CELL TUMOUR OF BONE. Orthop Procs. 2010 Jul 1;92-B(SUPP_III):440-440. https://doi.org/10.1302/0301-620X.92BSUPP_III.0920440c

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Abstract

Giant cell tumour of bone (GCTB) is an expansile osteolytic tumour of bone which contains numerous osteoclast-like giant cells. GCTB is a locally aggressive tumour which can cause extensive bone destruction that can be difficult to control surgically, up to 35% of cases recurring after simple curettage. Bisphosphonates are anti-resorptive agents that have proved effective in the treatment of a number of osteolytic conditions.

In keeping with its known effect on osteoclasts, we found that the aminobisphosphonate zoledronate abolished in vitro lacunar resorption in cultures of osteoclasts isolated from GCTB. The effect of zoledronate and other bisphosphonates on 15 cases of recurrent primary GCTB, four of which had metastasised to the lung, was assessed clinically. Most recurrent tumours did not exhibit progressive enlargement and, in some cases, both primary and metastatic GCTBs showed a degree of radiological improvement following treatment However, tumours did not diminish in size and, in some cases, no apparent treatment effect was noted.

Our findings provide in vitro evidence for the use of bisphosphonates to inhibit the progressive osteolysis associated with GCTB. In vivo, these agents produced a degree of clinical and radiological improvement in some cases. This study reports results from three European centres where bisphosphonates are being used to treat recurrent GCTB and highlights the fact that these centres are all employing different clinical indications and different regimes of bisphosphonate treatment. Bisphosphonates have significant side effects and indications for treatment and standardisation of drug type and dosage regimes (and measurement of agreed outcome measures to determine treatment efficacy) should be established before these agents are included as part of a treatment protocol to control GCTB tumour growth and osteolysis.

Correspondence should be addressed to Professor Stefan Bielack, Olgahospital, Klinikum Stuttgart, Bismarkstrasse 8, D-70176 Stuttgart, Germany. Email: s.bielack@klinikum_stuttgart.de