Phase II study of everolimus in patients with locally advanced or metastatic transitional cell carcinoma of the urothelial tract: clinical activity, molecular response, and biomarkers

Seront, Emmanuel; Rottey, Sylvie; Sautois, Brieuc; Kerger, Joseph; D’Hondt, Lionel; Verschaeve, Vincent; Canon, Jean Luc; Dopchie, Catherine; Vandenbulcke, Jean-Marie; Whenham, Nicolas; Goeminne, Jean-Charles; Clausse, Marylene; Verhoeven, Didier; Glorieux, Philippe; Branders, Samuel; Dupont, Pierre; Schoonjans, Joelle M.; Feron, Olivier; Machiels, Jean‐Pascal

doi:10.1093/annonc/mds057

Cited by 122 publications

(98 citation statements)

References 43 publications

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“…Là encore, les données cliniques pour proposer une intervention thérapeutique sur ces aberrations spécifiques sont limitées. Par exemple, l'efficacité des inhibiteurs de mTOR en cas de perte de la protéine (phosphatase) PTEN est très discutée (16,17). Les gains ou les pertes des gènes ne se traduisent d'ailleurs pas systématiquement par des surexpressions ou des absences des protéines correspondantes.…”

Section: Conditions Pre-analytiques Et Resultats D'analyseunclassified

“…De façon simpliste, l'amplification et/ou la mutation activatrice d'un gène dit « pilote fort » est à privilégier comme cible. A l'opposé, l'activation supposée d'une voie (par exemple PI3K/AKT/mTOR) offre des opportunités de traitement (inhibiteurs de PI3K, d'AKT ou de mTOR), mais n'est que rarement prédictive de l'efficacité de ces traitements (16)(17)(18). Dans les deux cas, hors indication approuvée formellement, les patients doivent être traités dans le cadre de protocoles de recherche clinique formalisés.…”

Section: Importance Des Rcp Moleculairesunclassified

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New Perspectives in Medical Oncology : Molecular Medicine and its Perspectives

Blay

Trédan

Pérol

2017

IJMS

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RESUMELa médecine moléculaire du cancer s'appuie sur l'identification d'anomalies génomique de l'ADN des cellules tumorales, permettant de guider le traitement des patients, en choisissant des inhibiteurs agissant sur les protéines mutées codées par les gènes mutés. Cependant, on assiste depuis 10 ans à l'émergence très rapide d'un nouveau corpus de connaissance décrivant les anomalies génomiques des cellules cancéreuses au sein des programmes internationaux comme ICGC ou TCGA, permettant de déboucher sur de nouvelles classifications nosologiques mais démontrant aussi l'extrême complexité et variabilité clonale des cellules cancéreuses chez le patient humain. Il s'agit désormais d'utiliser ces données nouvelles de manière efficace. Ceci requiert la constitution de plateformes de diagnostic explorant progressivement avec une plus grande profondeur les anomalies moléculaire de chaque patient individuel, et l'organisation de réunions de concertation pluridisciplinaires moléculaire permettant d'intégrer ces données au contexte clinique et global du patient, et requérant la contribution croissante des bio-informaticiens. Ce court article fait le point sur l'évolution de cette médecine moléculaire. ABSTRACTThe molecular medicine of cancer is based on the identification of genomic abnormalities in the DNA of tumor cells, guiding the treatment of patients, by choosing inhibitors acting on the mutated proteins encoded by the mutated genes. However, for the last 10 years, there has been a very rapid emergence of a new corpus of knowledge describing the genomic abnormalities of cancer cells in international programs such as ICGC or TCGA, leading to new nosological classifications, but also showing the extreme complexity and clonal variability of cancer cells in the human patient. The optimal use of this body of new data effectively. This requires 1) the construction of diagnostic platforms progressively exploring with greater depth the molecular anomalies of each individual patient and 2) the organization of multidisciplinary molecular consultation meetings to integrate these data into the clinical and global context of the patient. This evolution will also require a growing contribution of bio-informatics. This short article provides a short update on the evolution of this molecular medicine of cancer.

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Section: Conditions Pre-analytiques Et Resultats D'analyseunclassified

Section: Importance Des Rcp Moleculairesunclassified

New Perspectives in Medical Oncology : Molecular Medicine and its Perspectives

Blay

Trédan

Pérol

2017

IJMS

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“…Indeed, preclinical studies using bladder cancer cell models or xenografted mice demonstrated that inhibition of mTOR by everolimus inhibited bladder cancer cell growth in vitro and in xenografted mice [19]. Subsequently, clinical trials evaluating the mTOR inhibitors everolimus or temsirolimus in this population of patients have been performed but failed to meet their primary objectives despite some prolonged responses [26,27,29]. The results of our multicenter single-arm phase II trial showed for the first time a clinical benefit of temsirolimus for the treatment of patients with relapsed bladder cancer after first-line chemotherapy.…”

Section: Discussionmentioning

confidence: 99%

“…In terms of toxicity, both trials showed a similar safety profile with equivalent rates (20%) of grade 3-4 adverse events (mainly hematologic toxicity and fatigue), indicating an acceptable tolerance in patients with an ECOG status ≤2 and a rate of visceral metastases of approximately 80%, which is highly representative of such kind of population. The first phase II trial with everolimus reported a clinical activity with a 2-month non progression rate of 27% in a cohort of 28 assessable patients [26]. The second study was performed in a larger cohort of 45 patients and reported a 2-month non-progression rate of 51%, which is almost identical to the results of our study, despite the enrollment of a significant proportion of patients who received 2 or more additional lines of treatment following first line platinum-based chemotherapy [27].…”

Section: Discussionmentioning

confidence: 99%

“…Two phase II trials have been conducted with everolimus in patients with urothelial cancer who were refractory to first line platinum-based chemotherapy and showed mild antitumor activity [26,27]. The study of Seront et al reported a prevalence of PTEN loss in nonresponder patients, 21 and only few prolonged responses were associated with the presence of specific mutations of the TSC1 gene [28].…”

Section: Introductionmentioning

confidence: 99%

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Safety and efficacy of temsirolimus as second-line treatment for patients with recurrent bladder cancer.

Houédé

Roubaud

Mahammedi

et al. 2015

JCO

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Background: Bladder cancer is the 7th cause of death from cancer in men and 10th in women. Metastatic patients have a poor prognosis with a median overall survival of 14 months. Until recently, vinflunine was the only secondline chemotherapy available for patients who relapse. Deregulation of the PI3K/AKT/mTOR pathway was observed in more than 40% of bladder tumors and suggested the use of mTOR as a target for the treatment of urothelial cancers. Methods: This trial assessed the efficacy of temsirolimus in a homogenous cohort of patients with recurrent or metastatic bladder cancer following first-line chemotherapy. Efficacy was measured in terms of non-progression at two months according to the RECIST v1.1 criteria. Based on a two-stage optimal Simon's design, 15 non-progressions out of 51 evaluable patients were required to claim efficacy. Patients were treated at a weekly dose of 25 mg IV until progression, unacceptable toxicities or withdrawal.

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