Ovarian Neoplasm Clinical Trial
Official title:
Survival Data and Characteristics of Finisterian Patients Treated With PARP Inhibitors for Ovarian Cancer Between 2014 and 2019. Study of Efficacy and Safety Based on Finisterian Data Compared to Data in the Literature.
Ovarian cancer is a relatively uncommon but serious disease. It ranks 10th for female cancers, 5th for mortality, and its origin is still imperfectly known. It has a silent history for a long time, is often diagnosed late, and the prognosis is poor with a high relapse rate. It is therefore necessary to assess and prevent the risk of relapse, in order to establish a diagnosis as early as possible, and thus set up the appropriate treatment. Poly-ADP-Ribose Polymerase (PARP) inhibitors such as OLAPARIB and NIRAPARIB are effective in maintenance to prevent the risk of relapse in patients with recurrent platinum-sensitive ovarian cancer, as proved by recent data from the medical literature. Nevertheless, there may be a difference between "real life" and clinical trial data. Thus, the objective of this cohort is to assess whether the efficacy and safety of PARP inhibitors is the same in Finistère patients as in the scientific literature.
Ovarian cancer is a relatively uncommon but serious disease. It ranks 10th for female cancers
and 5th for mortality (4,720 new cases in France in 2017, for 3,111 deaths), and its origin
is still imperfectly known. Several risk factors have been identified, the main ones being
genetic (importance of heredity, BRCA mutations) and environmental (taking hormone
replacement therapy based on estrogen at menopause, exposure to tobacco, asbestos…).
Epithelial tumors are the most frequent (85%), with different subtypes: serous (40 to 50%);
endometrioid (20%); mucinous (15%); clear cell (5%); or with transitional, undifferentiated
and mixed cells. The classification used in clinical practice is the TNM classification which
establishes the stage of the disease (FIGO). Initial treatment is based on surgery and
chemotherapy. The standard scheme combines CARBOPLATIN and PACLITAXEL for 6 cycles. For
advanced stages, IIIB, IIIC and IV, BEVACIZUMAB can be administered every 3 weeks in
combination with CARBOPLATIN and PACLITAXEL, and is then continued as monotherapy for 15
months The management of recurrences depends on their time of occurrence. Before 6 months, it
is a resistance to platinum, a monochemotherapy without platinum is then indicated,
associated with BEVACIZUMAB, if it was not given initially and in the absence of
contraindication. After 6 months, polychemotherapy with platinum must be administered,
possibly associated with BEVACIZUMAB, again if it was not given initially and in the absence
of a contraindication. This treatment is then continued after stopping chemotherapy, until
progression or toxicity .The arrival of PARP (Poly-ADP-Ribose-Polymerase) inhibitors, such as
OLAPARIB, NIRAPARIB, or even RUCAPARIB, has considerably modified the treatment regimen of
these relapses known as "platinum-sensitive" These molecules act on the DNA repair system, in
synergy with the loss of BRCA function by tumor cells, causing significant genetic
instability leading to cell death. This is the principle of synthetic lethality. These
treatments will also in the very near future modify the management of patients with ovarian
cancer as soon as they are managed. In fact, the SOLO 1 study published in 2018 showed the
benefit of OLAPARIB prescribed as maintenance treatment in BRCA mutated patients, in complete
or partial response after chemotherapy based on platinum The PRIMA and VELIA studies,
published in 2019, have shown the effectiveness of NIRAPARIB and VELIPARIB respectively,
prescribed as maintenance therapy, regardless of the patients' BRCA status.The benefit of the
treatment was greater in the group of patients with a defect in homologous recombination.
Finally, the PAOLA study published in 2019, showed the benefit of OLAPARIB versus placebo, in
combination with BEVACIZUMAB, as maintenance treatment in patients with ovarian cancer in
full or partial response after chemotherapy with PLATINUM-PACLITAXEL-BEVACIZUMAB, regardless
of their BRCA status PARP inhibitors are effective in maintenance to prevent the risk of
relapse, in patients with recurrent ovarian cancer sensitive to platinum (relapse> 6 months
after the last course of platinum), as proved by recent data from the medical literature. On
the one hand, the SOLO 2 study showed an improvement in progression-free survival in patients
with a BRCA constitutional or somatic mutation, in relapse of platinum-sensitive ovarian
cancer, treated with OLAPARIB in maintenance (19.1 months versus 5.5 months) On the other
hand, the NOVA (2016) and ARIEL 3 (2017) studies showed an improvement in progression-free
survival in relapsed patients with platinum-sensitive ovarian cancer, treated with
maintenance by NIRAPARIB or by RUCAPARIB respectively, regardless of their mutational status
for BRCA (probable action on other homologous recombination pathways than BRCA, still unknown
to date) All these molecules are now part of our therapeutic arsenal, from the 2nd line of
treatment.
In this context of major progress in the management of ovarian cancer, we decided to set up a
Finistère study, aiming to analyze the characteristics and survival data of patients treated
with PARP inhibitor for a recurrent platinum-sensitive ovarian cancer, as well as their
tolerance to these treatments. This is a retrospective study, using data from Finistère in
comparison with data from the literature. Nevertheless, there may be a difference between
"real life" and clinical trial data. Thus, the objective of this cohort is to assess whether
the efficacy (survival) and safety (side effects) of PARP inhibitors is the same in Finistère
patients as in the scientific literature.
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