83 research outputs found
Tratamiento del osteosarcoma localizado de las extremidades
En la década de los setenta, la introducción de la quimioterapia preoperatoria en el
tratamiento del osteosarcoma proporcionó mejoras dramáticas en los resultados obtenidos a largo
plazo, en cuanto a la supervivencia libre de enfermedad y los procedimientos de salvación de miembros.
En el presente trabajo se describe la experiencia acumulada en el Instituto Rizzoli, con la aplicación
de varios protocolos activados sucesivamente. Igualmente, se describen los distintos factores
pronósticos, la necrosis inducida por quimioterapia, dosis/intensidad y niveles séricos de metotrexato.In the seventies, the introduction of preoperative chemotherapy in the treatment of
osteosarcoma dramatically improved the results in terms of disease-free survival and limb salvage
procedures. This paper reports the experience at the Rizzoli Institute showing the results obtained
with several successively activated protocols. Different prognostic factors, including chemotherapy
induced necrosis, dose/intensity, methotrexate serum concentration are also discussed
Proton pump inhibitor chemosensitization in human osteosarcoma: from the bench to the patients' bed.
BACKGROUND:
Major goals in translational oncology are to reduce systemic toxicity of current anticancer strategies and improve effectiveness. An extremely efficient cancer cell mechanism to avoid and/or reduce the effects of highly cytotoxic drugs is the establishment of an acidic microenvironment, an hallmark of all malignant tumors. The H\u2009+-rich milieu that anticancer drugs meet once they get inside the tumor leads to their protonation and neutralization, therefore hindering their access into tumor cells. We have previously shown that proton pump inhibitors (PPI) may efficiently counterattack this tumor advantage leading to a consistent chemosensitization of tumors. In this study, we investigated the effects of PPI in chemosensitizing osteosarcoma.
METHOD:
MG-63 and Saos-2 cell lines were used as human osteosarcoma models. Cell proliferation after pretreatment with PPI and subsequent treatment with cisplatin was evaluated by using erythrosin B dye vital staining. Tumour growth was evaluated in xenograft treated with cisplatin after PPI pretreatment. Subsequently, a multi-centre historically controlled trial, was performed to evaluate the activity of a pre-treatment administration of PPIs as chemosensitizers during neoadjuvant chemotherapy based on methotrexate, cisplatin, and adriamycin.
RESULTS:
Preclinical experiments showed that PPI sensitize both human osteosarcoma cell lines and xenografts to cisplatin. A clinical study subsequently showed that pretreatment with PPI drug esomeprazole leads to an increase in the local effect of chemotherapy, as expressed by percentage of tumor necrosis. This was particularly evident in chondroblastic osteosarcoma, an histological subtype that normally shows a poor histological response. Notably, no significant increase in toxicity was recorded in PPI treated patients.
CONCLUSION:
This study provides the first evidence that PPI may be beneficially added to standard regimens in combination to conventional chemotherapy
ErbB2 and bone sialoprotein as markers for metastatic osteosarcoma cells
Osteosarcoma is the most common malignant bone neoplasia occurring in young patients in the first two decades of life, and represents 20% of all primitive malignant bone tumours. At present, treatment of metastatic osteosarcoma is unsatisfactory. High-dose chemotherapy followed by CD34+ leukapheresis rescue may improve these poor results. Neoplastic cells contaminating the apheresis may, however, contribute to relapse. To identify markers suitable for detecting osteosarcoma cells in aphereses we analysed the expression of bone-specific genes (Bone Sialoprotein (BSP) and Osteocalcin) and oncogenes (Met and ErbB2) in 22 patients with metastatic osteosarcoma and six healthy stem cell donors. The expression of these genes in aphereses of patients affected by metastatic osteosarcoma was assessed by RT–PCR and Southern blot analysis. Met and Osteocalcin proved to be not useful markers since they are positive in aphereses of both patients with metastatic osteosarcoma and healthy stem cell donors. On the contrary, BSP was expressed at significant levels in 85% of patients. Moreover, 18% of patients showed a strong and significantly positive (seven to 16 times higher than healthy stem cell donors) ErbB2 expression. In all positive cases, neoplastic tissue also expressed ErbB2. Our data show that ErbB2 can be a useful marker for tumour contamination in aphereses of patients affected by ErbB2-expressing osteosarcomas and that analysis of Bone Sialoprotein expression can be an alternative useful marker
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