GIANT CELL TUMOUR OF BONE: RETROSPECTIVE ANALYSIS OF RISK FACTORS FOR LOCAL RECURRENCE

M.A.J. van de Sande; L. van der Heijden; M. Gibbons; P.D.S. Dijkstra

doi:10.1302/1358-992X.94BSUPP_XXX.BOOS2011-004

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GIANT CELL TUMOUR OF BONE: RETROSPECTIVE ANALYSIS OF RISK FACTORS FOR LOCAL RECURRENCE

British Orthopaedic Oncology Society (BOOS) - 2011 Annual Scientific Meeting

M.A.J. van de Sande
L. van der Heijden
M. Gibbons
P.D.S. Dijkstra

GIANT CELL TUMOUR OF BONE: RETROSPECTIVE ANALYSIS OF RISK FACTORS FOR LOCAL RECURRENCE

van de Sande M, van der Heijden L, Gibbons M, Dijkstra P. GIANT CELL TUMOUR OF BONE: RETROSPECTIVE ANALYSIS OF RISK FACTORS FOR LOCAL RECURRENCE. Orthop Procs. 2012;94-B(SUPP_XXX):4-4. doi:10.1302/1358-992X.94BSUPP_XXX.BOOS2011-004

van de Sande, M.A.J., et al. “GIANT CELL TUMOUR OF BONE: RETROSPECTIVE ANALYSIS OF RISK FACTORS FOR LOCAL RECURRENCE.” Orthopaedic Proceedings, vol. 94-B, no. SUPP_XXX, 2012, pp. 4-4., https://doi.org/10.1302/1358-992X.94BSUPP_XXX.BOOS2011-004

van de Sande, M., van der Heijden, L., Gibbons, M., & Dijkstra, P. (2012). GIANT CELL TUMOUR OF BONE: RETROSPECTIVE ANALYSIS OF RISK FACTORS FOR LOCAL RECURRENCE. Orthopaedic Proceedings, 94-B(SUPP_XXX), 4-4. https://doi.org/10.1302/1358-992X.94BSUPP_XXX.BOOS2011-004

van de Sande, M., van der Heijden, L., Gibbons, M. and Dijkstra, P. (2012) “GIANT CELL TUMOUR OF BONE: RETROSPECTIVE ANALYSIS OF RISK FACTORS FOR LOCAL RECURRENCE.” Orthopaedic Proceedings, 94-B(SUPP_XXX), pp. 4-4. Available at: https://doi.org/10.1302/1358-992X.94BSUPP_XXX.BOOS2011-004

van de Sande, M.A.J., L. van der Heijden, M. Gibbons, and P.D.S. Dijkstra. “GIANT CELL TUMOUR OF BONE: RETROSPECTIVE ANALYSIS OF RISK FACTORS FOR LOCAL RECURRENCE.” Orthopaedic Proceedings 94-B, no. SUPP_XXX (2012): 4-4. https://doi.org/10.1302/1358-992X.94BSUPP_XXX.BOOS2011-004

van de Sande M, van der Heijden L, Gibbons M, Dijkstra P. GIANT CELL TUMOUR OF BONE: RETROSPECTIVE ANALYSIS OF RISK FACTORS FOR LOCAL RECURRENCE. Orthop Procs. 2012 Jul 1;94-B(SUPP_XXX):4-4. https://doi.org/10.1302/1358-992X.94BSUPP_XXX.BOOS2011-004

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Abstract

Introduction

Local recurrence of Giant cell tumours of bone (GCT) is considered the main complication of surgical treatment (50%). Intra-lesional curettage with adjuvants like phenol or polymethylmethacrylate (PMMA) is recommended as initial treatment, decreasing the risk of recurrence. However, risk factors for local recurrence in skeletal GCT have not yet been firmly established and a golden standard for treatment remains controversial.

Aim of this study is identification of risk factors for recurrence in GCT, specifically after intra-lesional curettage with or without adjuvants.

Methods

In a retrospective single-institution study 191 patients treated for GCT between 1964 and 2009 were included. Mean follow-up was 111 months (range 12-415). The recurrence-free survival and hazards for different treatment strategies and various patient and tumour characteristics were determined.

Results

Overall risk of recurrence was 36.1% (n=66, 95% CI: 28.3-42.1). Recurrence rate after wide resection was 20%, after curettage with adjuvants 33% and after curettage alone 77%. Hogendoorn-grade III (Hazard Ratio: 5.7, p⋋0.001), localisation in axial skeleton (HR: 3.7, p⋋0,001), primary treatment in a non-specialised centre (HR: 2.8, p⋋0.001) and extension into soft tissue (HR: 2.0, p=0.02) were significant risk factors for local recurrence. Curettage with adjuvants proved superior to curettage alone (p⋋0.004 p=0.07, HR: 0.54), but the application of both PMMA and phenol did not present a significantly better outcome than PMMA alone (HR: 1.07, p=0.9).

Discussion

Of all possible risk factors only soft tissue extension and localisation in distal radius significantly influenced the risk of local recurrence for all treatments. We found that high-grade tumours and localisation in the axial skeleton were additional risk factors for local recurrence after intra-lesional surgery. Although wide resection increases morbidity, it can be the therapy of choice in high risk patients. Intra-lesional therapy can be advised for low risk patients using curettage adjuvants and PMMA.