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Orthopaedic Proceedings
Vol. 92-B, Issue SUPP_III | Pages 436 - 436
1 Jul 2010
Ługowska I Woźniak W Ambroszkiewicz J Gajewska J Szamotulska K
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Serum level of the extracellular domain of HER-2 (ECD/HER2) has been suggested to be a tumor marker in breast cancer. The aim of this study was to assess the prognostic value of baseline level of ECD/HER2 and changes in levels over time in children and adults with osteosarcoma during chemotherapy.

Materials and methods: We analysed 33 newly-diagnosed osteosarcoma patients treated at the Department of Paediatric Oncological Surgery of the Institute of Mother and Child, Warsaw, Poland between 2005–2008. Patients characteristics: age 8–18 years (median 15); staging at diagnosis: disease localised (18) and dissemination (15); disease progression (13); deaths (6). Follow-up: 8–37 months (median 19). ECD/HER2 was measured in 118 serum samples using a validated ELISA kit: at the time of diagnosis (1), after preoperative chemotherapy (2), 2 weeks after surgery (3) and 3–6 moths after surgery (4).

Results: The baseline level of ECD/HER-2 in serum ranged 3.8–34.4 ng/mL (median 5). The elevated baseline ECD/HER2 was associated with decreased progression free survival (ECD/HER2 ng/mL> 5 vs ECD/HER2 ng/mL≤5: 44% vs 77%; p=0.039) and decreased overall survival (ECD/HER2 ng/mL> 5 vs ECD/HER2 ng/mL≤5: 69% vs 94%, p=0.115). The concentration of ECD/HER2> 6 ng/ml during treatment (specially postoperative chemotherapy) was associated with early disease progression (p=0.095).

Conclusions: The high level of ECD/HER2 at the time of diagnosis may be a marker of poor prognosis in osteosarcoma. Additionally, we suggest that changes of this marker concentration over time could be helpful for treatment monitoring.


Orthopaedic Proceedings
Vol. 92-B, Issue SUPP_III | Pages 435 - 435
1 Jul 2010
Ługowska I Woźniak W Klepacka T Michalak E Karwacki M Rychłowska-Pruszyńska M Szamotulska K
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In osteosarcoma, treatment guidelines recommend standard chemotherapy regardless of severity of disease. Treatment individualization will minimize risk of failure and adverse effects, specially in patients who have good prognosis. Therefore, there is a pressing clinical need to develop a risk adapted strategies and to adjust chemotherapy to prognostic factors.

Aim: to asses usefulness of Classification and Regression Tree Analysis (C& RT) for stratifying patients with localised osteosarcoma to the risk groups according to clinical and biological markers.

Material and methods: 100 patients with localised osteosarcoma were included, aged 5–23 years (mean 14), with extremity localisation of the primary tumour. Follow up – at least 5 years since a date of diagnosis. We analysed clinical prognostic factors (tumour size, pathological fracture, alkaline phosphatase, age), histological prognostic factors (% of viable tumour cells after pre-operative chemotherapy, subtype of osteosarcoma and its aggressiveness) and biological factors (expression of VEGF, Ki-67, Topoisomerase II alpha and P glycoprotein). The expressions of proteins were measured immunohistochemically in biopsy samples. C& RT model included all described above factors.

Results: C& RT analysis revealed that the most important prognostic factors in localised osteosarcoma were: VEGF, Topoisomerase II alpha and tumour size. This markers were included into the risk classification and three risk groups were proposed: with poor prognosis (n=13) – 5 year OS 31%, moderate (n=57) – 5 year OS 63% and with good prognosis (n=30) – 5 year OS 93%), P=0.000.

Conclusion: C& RT is useful method for stratifying patients with osteosarcoma to risk groups. The stratification should include biological and clinical prognostic markers.