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Radioimmunotherapy in advanced ovarian cancer: Is there a role for pre-targeting with 90Y-biotin?

Authors :
Grana, C
Bartolomei, M
Handkiewicz, D
Rocca, P
Bodei, L
Colombo, N
Chinol, M
Mangioni, C
Malavasi, F
Paganelli, G
Paganelli, G.
COLOMBO, NICOLETTA
Grana, C
Bartolomei, M
Handkiewicz, D
Rocca, P
Bodei, L
Colombo, N
Chinol, M
Mangioni, C
Malavasi, F
Paganelli, G
Paganelli, G.
COLOMBO, NICOLETTA
Publication Year :
2004

Abstract

Despite recent advances in the management of ovarian cancer, this tumor remains the leading cause of death among gynecologic malignancies. Moreover, advanced ovarian carcinoma has a poor prognosis, thus requiring new therapeutic modalities. Previous studies have indicated a survival advantage for ovarian cancer patients (pts) treated with radioimmunotherapy (RIT). Pre-targeting RIT, based on the avidin–biotin system, has been the objective of previous studies performed by our group. Patients and methods. In the present study, the therapeutic efficacy and toxicity of RIT in 38 advanced ovarian cancer patients have been retrospectively evaluated. RIT was performed according to the following three-step protocol: biotinylated monoclonal antibodies (MoAb) and avidin were intraperitoneally (ip) injected (1st and 2nd step), and 12–18 h later 90Y-labeled biotin either iv or ip was injected as 3rd step. Sixteen out of 38 patients were treated by intraperitoneal injection only, whereas other 22 pts received the combined treatment (ip + iv); the dose range was 10–100 mCi of 90Y-biotin. Results. Both of the two therapy regimens were well tolerated; no acute side effects were observed. Two patients (5%) showed temporary hematological grade III–IV toxicity. As regards to the therapeutic efficacy, in the ip group we observed 6% of objective tumor reduction, stabilization in 31% of pts, and progression in 50%. In the group of combined treatment, 9% of patients achieved objective responses, 32% showed stable disease, and 41% had a progression. Conclusions. These data show the excellent tolerability (maximum tolerated dose (MTD) has not been determined yet) and the potential therapeutic role of RIT in advanced ovarian cancer. Patients with minimal residual disease would probably take the best advantages of RIT with 90Y-biotin (electrons). These data warrant further prospective studies

Details

Database :
OAIster
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1308896231
Document Type :
Electronic Resource