Muscle Invasive Bladder Cancer Clinical Trial
Official title:
Identification and Treatments of Basal Like Bladder Cancer (Study on Human Tumor Samples and Animal Models)
Muscle invasive (MIBC) and/or metastatic bladder cancer is associated with poor prognosis and no target therapies for this pathology are currently validated. By 40 gene expression signature realized on frozen samples, we have previously identified an aggressive sub-class of MIBC, called basal. This sub-class (20% of MIBC) showed strong EGFR dependence in vitro and in vivo (Rebouissou et al. Science Translational Medicine 2014). This observation suggests a possible response to EGFR targeted therapy in patients of this subgroup. Our aim is to establish a standard diagnostic tool to differentiate the basal subtype of bladder cancer and evaluate the effect of anti-EGFR therapy, by analyzing previous clinical trial (GETUG19) and preclinical models, which compare the classical chemotherapy to anti-EGFR associated chemotherapy.
The aim of this study is:
1. To validate a diagnostic test for formalin-fixed paraffin-embedded (FFPE) samples by
Nanostring technology, using the 40 genes signature as reference. First, we will
compare frozen and FFPE tissues (n=120), to establish a transcriptional signature in
FFPE samples. Secondly, to further characterize basal subtype of bladder cancer, we
will study the mutational and gain/loss landscape and immunohistochemistry markers in a
new series of tumors after classifying them by our gene signature (n=510). These
characteristics will be included in a new signature by defining the optimal prediction
discrimination AIC et Net Reclassification Index.
2. To assess the prognosis after cisplatine treatment in 510 patients treated by
cystectomy with or without adjuvant chemotherapy (pT2/pT3/pT4, N0 or N+) and in another
multicentric series of 188 patients treated by cystectomy and adjuvant chemotherapy
(pT3/pT4 et/ou N+). Uni and multi variant analysis will be realized by adjusted Cox
model, and the added value of basal subtype as compared to standard prognostic factors
will be evaluated. The propensity score will be realized to assess the association of
basal subtype and response to chemotherapy. The anti-EGFR response will be analyzed in
the clinical trial GETUG19 which uses Panitumumab in patients with metastatic
urothelial carcinomas (n=93)
3. To study the treatment response in preclinical models. We characterized previously
preclinical murine models derived from xenografts of MIBC (n=14 and new xenografts will
be added). We will study the effect of anti-EGFR alone or in combination with
chemotherapy in basal and non basal subtypes of xenografts.
By this study we will be able to better characterize the basal subtype of bladder cancer and
confirm its aggressive behaviour as compared to other subtypes of MIBC. These results will
further help to establish new clinical trials which include anti-EGFR in patients of basal
subtype.
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