Bevacizumab plus microtubule targeting agents in heavily pre-treated ovarian cancer patients: a retrospective study - 27/03/15

Doi : 10.1684/bdc.2011.1436

Irène Asmane ^⁎,¹ , Jean-Emmanuel Kurtz ¹, Agathe Bajard ⁸, Jean-Paul Guastalla ², Pierre Meeus ³, Olivier Tredan ², Intidhar Labidi Galy ², Isabelle Moullet ⁴, Philippe Ardisson ⁴, Lionel Vincent ⁵, David Coeffic ⁶, Armelle Dufresne ⁷, Jean-Pierre Bergerat ¹, Isabelle Ray-Coquard ²
¹ CHU Hautepierre, Department of Oncology & Hematology, 1, avenue Molière, 67000 Strasbourg, France
² Centre Léon-Bérard, Department of Oncology, 69008 Lyon, France
³ Centre Léon-Bérard, Department of Surgical Oncology, 69008 Lyon, France
⁴ Clinique de la Sauvegarde, Department of Oncology, 69009 Lyon, France
⁵ Centre hospitalier régional de Roannes, Medical Oncology Unit, 42300 Roannes, France
⁶ Institut Daniel-Hollard, groupe hospitalier mutualiste Grenoble, Medical Oncology Unit, 38000 Grenoble, France
⁷ Centre hospitalier régional de Chambéry, Department of Oncology & Hematology, 73000 Chambéry, France
⁸ Centre Léon-Bérard, Department of Statistics, 69008 Lyon, France

^*Tirés à part.

Abstract

Objectives

As vascular endothelial growth factor (VEGF) is expressed in ovarian cancer, we assessed the efficacy and safety of bevacizumab (a monoclonal antibody targeting VEGF) plus microtubule targeting agents for heavily pre-treated ovarian carcinoma patients.

Methods

We retrospectively reviewed 43 patients with recurrent epithelial ovarian carcinoma. Combined treatment included bevacizumab with paclitaxel in 32 (74%), docetaxel in 10 (23%), and vinorelbine in one (2.3%) patients, respectively.

Results

The median number of combined treatment was six cycles (range 1-29). On RECIST criteria, the objective response rate (ORR) was 40% (16% CR and 24% PR). Clinical benefit (complete response [CR] plus partial response [PR] and stable disease [SD] lasting≥3 months) was 74% (CI95%: 46.7-77%). Median duration of treatment and overall survival were 3.9 months (range 0.2-14.4 months) and 20.1 months (CI95%: 13.8-20.1) respectively. No toxic death was reported. Grade 3-4 toxicity occurred in 30% of patients. Gastrointestinal perforations and fistula occurred in 3 (7%) and 6 (14%) patients, respectively.

Conclusions

Although being active in terms of ORR, bevacizumab plus microtubule targeting agents – mainly taxanes – leads to a high rate of gastro-intestinal perforations and fistula in heavily pre-treated ovarian carcinoma patients.

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Key words : bevacizumab, microtubule targeting agents, ovarian cancer, gastro-intestinal perforations

Plan

Evaluation of efficacy and toxicity

Statistical analysis

Results

Patients characteristics

Treatment schedule

Tumour response

Factors affecting response to therapy

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Vol 98 - N° 9

P. E80-E89 - septembre 2011 Retour au numéro

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Bevacizumab plus microtubule targeting agents in heavily pre-treated ovarian cancer patients: a retrospective study - 27/03/15

Abstract

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Plan

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