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Brain Metastases from an Ovarian Cancer, Single Centre Study

Brain Metastases from an Ovarian Cancer, Single Centre Study. F Azam, H Wong, J O’Hagan, R Lord, JA Green Clatterbridge Centre for Oncology , Clatterbridge Road, Bebington, Wirral Merseyside CH63 4JY. Introduction

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Brain Metastases from an Ovarian Cancer, Single Centre Study

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  1. Brain Metastases from an Ovarian Cancer, Single Centre Study F Azam, H Wong, J O’Hagan, R Lord, JA Green Clatterbridge Centre for Oncology , Clatterbridge Road, Bebington, Wirral Merseyside CH63 4JY Introduction Brain is a rare site of metastases from an ovarian primary. Limited data are available on prognostic factors, standard treatment and survival. As overall survival has increased with improvement in chemotherapy for the primary ovarian cancer more patients will present with brain metastases. Knowledge of clinical prognostic factors would help the management of patients with brain metastases. Aims The aim of this study is to evaluate the impact of clinical factors and treatment modalities on survival in patients with brain metastases from an ovarian cancer treated at the single UK oncology centre. Methods Analysis of a prospective electronic database of patients with brain metastases from an ovarian primary treated at the Clatterbridge Centre for Oncology serving a population of 3 millions. Kaplan-Meier survival estimates were used to calculate the survival and Cox regression was used to identify the variables associate with survival. Clinical variables and treatment modalities studied are summarised in table 1 and table 2 respectively. Results A total of 20 patients with brain metastases from ovarian primary were treated with radiotherapy (RT) from Apr2001-Feb2011. Median age at occurrence of brain metastases was 55 years. The median time from primary diagnosis to occurrence of brain metastases was 20 months (range 1-208 months). Median overall survival from diagnosis of brain metastases was 9 months (95% CI 6.9-11.0 months), Figure 1. On univariate analysis, poor ECOG performance status (p=0.029) and platinum resistance (p=0.002) were the most significant adverse variables identified. Whilst platinum resistance and advance FIGO staging were significant adverse prognostic factors on multi-variate analysis. Median survival was 13 months for platinum sensitive patients and 6 months for platinum resistant patients, p=0.001, Figure 2. All patients were treated with RT. Only 6(30%) patients had surgical resection and 7(35%) patients received chemotherapy (CT). Patients treated with multimodal therapy had a median survival of 14 months (N=11) and 8 months for RT only (N=9), p=0.011, Figure 3. Three patients were still alive 2 months, 7 months and 42 months after diagnosis of brain metastases. Figure 1 : Overall Survival from diagnosis of brain metastases Figure 2: Overall Survival by Platinum Sensitivity Conclusion Platinum sensitivity is an important prognostic factor in patients with brain metastases from an ovarian primary tumour . Multimodal therapy using surgery, radiotherapy and chemotherapy should be considered where feasible. References 1.Geisler JP, Geisler HE. Brain metastases in epithelial ovarian carcinoma. Gynecol oncol 1995;57(2):246-249 2. Sehouli J, Pietzner K, Hartner P et al. Prognostic role of platinum sensitivity in patients with brain metastases from ovarian cancer: results of a German multicenter study. Annals of oncology 2010;21:2201-2205. Table 1 : Patient Characteristics Figure 3: Overall Survival by Treatment Modalities Table 2 : Treatment Modalities

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