Your search keyword '"Espié, Marc"' showing total 10 results

1. 18FDG-PET/CT and molecular markers to predict response to neoadjuvant chemotherapy and outcome in HER2-negative advanced luminal breast cancers patients

Author

de Cremoux, Patricia, Resche-Rigon, Matthieu, Sotiriou, Christos, Groheux, David DG, Biard, Lucie, Poirot, Brigitte, Bertheau, Philippe, Teixeira, Luis, Lehmann-Che, Jacqueline, Bouhidel, Fatiha Amira, Merlet, Pascal, Espié, Marc, de Cremoux, Patricia, Resche-Rigon, Matthieu, Sotiriou, Christos, Groheux, David DG, Biard, Lucie, Poirot, Brigitte, Bertheau, Philippe, Teixeira, Luis, Lehmann-Che, Jacqueline, Bouhidel, Fatiha Amira, Merlet, Pascal, and Espié, Marc

Abstract

Background: The efficacy of neoadjuvant chemotherapy regimens in advanced luminal breast cancer patients is difficult to predict. Intrinsic properties of breast tumors, including altered gene expression profile and dynamic evaluation of metabolic properties of tumor cells using positron emission tomography/computed tomography (PET/CT) of tumor cells, have been identified to guide patient's prognosis. The aim of this study is to determine if both analyses may improve the prediction of response to neoadjuvant chemotherapy in ER-positive / HER2-negative breast cancers (BCs) patients. Methods: We used metabolic PET parameters, at diagnosis and after two cycles of chemotherapy and proliferation gene expression profile on biopsy at diagnosis, in particular, the genomic grade index (GGI) analyzed by reverse transcription and quantitative polymerase chain reaction (RT-qPCR). The pathological response was the surrogate endpoint. Results: The change of FDG uptake between baseline PET and interim PET after 2 cycles of neoadjuvant chemotherapy (ΔSUVmax) was highly associated with pCR (p=0.008). We also observed an ability of P53 mutated status (p=0.042), in addition to histological grade (p=0. 0004), and PR expression (p=0.01) to predict pCR in ERpositive BCs, whereas no proliferation marker predicted pCR (P=0.39 for GGI). Finally, only ΔSUVmax was significantly associated with event free survival (p=0.047). Conclusions: Our results confirm the predictive and prognostic value of tumor ΔSUVmax in ER-positive /HER2-negative advanced BCs patients. These findings can be helpful to select high-risk patients within trials investigating novel treatment strategies., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2018

2. Ipatasertib plus paclitaxel versus placebo plus paclitaxel as first-line therapy for metastatic triple-negative breast cancer (LOTUS): a multicentre, randomised, double-blind, placebo-controlled, phase 2 trial.

Author

Kim, Sung-Bae, Kim, Sung-Bae, Dent, Rebecca, Im, Seock-Ah, Espié, Marc, Blau, Sibel, Tan, Antoinette R, Isakoff, Steven J, Oliveira, Mafalda, Saura, Cristina, Wongchenko, Matthew J, Kapp, Amy V, Chan, Wai Y, Singel, Stina M, Maslyar, Daniel J, Baselga, José, LOTUS investigators, Kim, Sung-Bae, Kim, Sung-Bae, Dent, Rebecca, Im, Seock-Ah, Espié, Marc, Blau, Sibel, Tan, Antoinette R, Isakoff, Steven J, Oliveira, Mafalda, Saura, Cristina, Wongchenko, Matthew J, Kapp, Amy V, Chan, Wai Y, Singel, Stina M, Maslyar, Daniel J, Baselga, José, and LOTUS investigators

Abstract

BackgroundThe oral AKT inhibitor ipatasertib is being investigated in cancers with a high prevalence of PI3K/AKT pathway activation, including triple-negative breast cancer. The LOTUS trial investigated the addition of ipatasertib to paclitaxel as first-line therapy for triple-negative breast cancer.MethodsIn this randomised, placebo-controlled, double-blind, phase 2 trial, women aged 18 years or older with measurable, inoperable, locally advanced or metastatic triple-negative breast cancer previously untreated with systemic therapy were recruited from 44 hospitals in South Korea, the USA, France, Spain, Taiwan, Singapore, Italy, and Belgium. Enrolled patients were randomly assigned (1:1) to receive intravenous paclitaxel 80 mg/m2 (days 1, 8, 15) with either ipatasertib 400 mg or placebo once per day (days 1-21) every 28 days until disease progression or unacceptable toxicity. Randomisation was by stratified permuted blocks (block size of four) using an interactive web-response system with three stratification criteria: previous (neo)adjuvant therapy, chemotherapy-free interval, and tumour PTEN status. The co-primary endpoints were progression-free survival in the intention-to-treat population and progression-free survival in the PTEN-low (by immunohistochemistry) population. This ongoing trial is registered with ClinicalTrials.gov (NCT02162719).FindingsBetween Sept 2, 2014, and Feb 4, 2016, 166 patients were assessed for eligibility and 124 patients were enrolled and randomly assigned to paclitaxel plus ipatasertib (n=62) or paclitaxel plus placebo (n=62). Median follow-up was 10·4 months (IQR 6·5-14·1) in the ipatasertib group and 10·2 months (6·0-13·6) in the placebo group. Median progression-free survival in the intention-to-treat population was 6·2 months (95% CI 3·8-9·0) with ipatasertib versus 4·9 months (3·6-5·4) with placebo (stratified hazard ratio [HR] 0·60, 95% CI 0·37-0·98; p=0·037) and in the 48 patients with PTEN-low tumours, median progression-free s

Published

2017

3. Distinct tumor protein p53 mutants in breast cancer subgroups.

Author

Dumay, Anne, Feugeas, Jean-Paul, Wittmer, Evelyne, Lehmann-Che, Jacqueline, Bertheau, Philippe, Espié, Marc, Plassa, Louis-François, Cottu, Paul, Marty, Michel, Andre, Fabrice, Sotiriou, Christos, Pusztai, Lajos, de Thé, Hugues, Dumay, Anne, Feugeas, Jean-Paul, Wittmer, Evelyne, Lehmann-Che, Jacqueline, Bertheau, Philippe, Espié, Marc, Plassa, Louis-François, Cottu, Paul, Marty, Michel, Andre, Fabrice, Sotiriou, Christos, Pusztai, Lajos, and de Thé, Hugues

Abstract

Tumor protein p53 (TP53) is mutated in approximately 30% of breast cancers, but this frequency fluctuates widely between subclasses. We investigated the p53 mutation status in 572 breast tumors, classified into luminal, basal and molecular apocrine subgroups. As expected, the lowest mutation frequency was observed in luminal (26%), and the highest in basal (88%) tumors. Luminal tumors showed significantly higher frequency of substitutions (82 vs. 65%), notably A/T to G/C transitions (31 vs. 15%), whereas molecular apocrine and basal tumors presented much higher frequencies of complex mutations (deletions/insertions) (36 and 33%, respectively, vs. 18%). Accordingly, missense mutations were significantly more frequent in luminal tumors (75 vs. 54%), whereas basal tumors displayed significantly increased rates of TP53 truncations (43 vs. 25%), resulting in loss of function and/or expression. Interestingly, as basal tumors, molecular apocrine tumors presented with a high rate of complex mutations, but paradoxically, these were not associated with increased frequency of p53 truncation. As in luminal tumors, this could reflect a selective pressure for p53 gain of function, possibly through P63/P73 inactivation. Collectively, these observations point not only to different mechanisms of TP53 alterations, but also to different functional consequences in the different breast cancer subtypes., JOURNAL ARTICLE, FLWIN, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2013

4. Distinct tumor protein p53 mutants in breast cancer subgroups.

Author

Dumay, Anne, Feugeas, Jean-Paul, Wittmer, Evelyne, Lehmann-Che, Jacqueline, Bertheau, Philippe, Espié, Marc, Plassa, Louis-François, Cottu, Paul, Marty, Michel, Andre, Fabrice, Sotiriou, Christos, Pusztai, Lajos, de Thé, Hugues, Dumay, Anne, Feugeas, Jean-Paul, Wittmer, Evelyne, Lehmann-Che, Jacqueline, Bertheau, Philippe, Espié, Marc, Plassa, Louis-François, Cottu, Paul, Marty, Michel, Andre, Fabrice, Sotiriou, Christos, Pusztai, Lajos, and de Thé, Hugues

Abstract

Tumor protein p53 (TP53) is mutated in approximately 30% of breast cancers, but this frequency fluctuates widely between subclasses. We investigated the p53 mutation status in 572 breast tumors, classified into luminal, basal and molecular apocrine subgroups. As expected, the lowest mutation frequency was observed in luminal (26%), and the highest in basal (88%) tumors. Luminal tumors showed significantly higher frequency of substitutions (82 vs. 65%), notably A/T to G/C transitions (31 vs. 15%), whereas molecular apocrine and basal tumors presented much higher frequencies of complex mutations (deletions/insertions) (36 and 33%, respectively, vs. 18%). Accordingly, missense mutations were significantly more frequent in luminal tumors (75 vs. 54%), whereas basal tumors displayed significantly increased rates of TP53 truncations (43 vs. 25%), resulting in loss of function and/or expression. Interestingly, as basal tumors, molecular apocrine tumors presented with a high rate of complex mutations, but paradoxically, these were not associated with increased frequency of p53 truncation. As in luminal tumors, this could reflect a selective pressure for p53 gain of function, possibly through P63/P73 inactivation. Collectively, these observations point not only to different mechanisms of TP53 alterations, but also to different functional consequences in the different breast cancer subtypes., JOURNAL ARTICLE, FLWIN, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2013

5. Cyclophosphamide dose intensification may circumvent anthracycline resistance of p53 mutant breast cancers.

Author

Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Mazouni, Chafika, Giacchetti, S, Turpin, Elisabeth, Espié, Marc, Plassa, Louis-François, Marty, Michel, Bertheau, Philippe, Sotiriou, Christos, Piccart-Gebhart, Martine, Symmans, W Fraser, Pusztai, Lajos, de Thé, Hugues, Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Mazouni, Chafika, Giacchetti, S, Turpin, Elisabeth, Espié, Marc, Plassa, Louis-François, Marty, Michel, Bertheau, Philippe, Sotiriou, Christos, Piccart-Gebhart, Martine, Symmans, W Fraser, Pusztai, Lajos, and de Thé, Hugues

Abstract

The predictive value of p53 for the efficacy of front-line anthracycline-based chemotherapy regimens has been a matter of significant controversy. Anthracyclines are usually combined with widely different doses of alkylating agents, which may significantly modulate tumor response to these combinations. We analyzed three series of de novo stage II-III breast cancer patients treated front line with anthracycline-based regimens of various cyclophosphamide dose intensities: 65 patients with estrogen receptor (ER)(-) tumors treated with anthracyclines alone (Institut Jules Bordet, Brussels), 51 unselected breast cancer patients treated with intermediate doses of cyclophosphamide (MD Anderson Cancer Center, Houston, TX), and 128 others treated with a dose-dense anthracycline-cyclophosphamide combination (St. Louis, Paris). After chemotherapy and surgery, pathologic complete response (pCR) was evaluated. p53 status was determined by a yeast functional assay on the pretreatment tumor sample. In a multivariate analysis of the pooled results, a lack of ER expression and high-dose cyclophosphamide administration were associated with a higher likelihood of pCR. A sharp statistical interaction was detected between p53 status and cyclophosphamide dose intensity. Indeed, when restricting our analysis to patients with ER(-) tumors, we confirmed that a mutant p53 status was associated with anthracycline resistance, but found that p53 inactivation was required for response to the dose-intense alkylating regimen. The latter allowed very high levels of pCR in triple-negative tumors. Thus, our data strongly suggest that cyclophosphamide dose intensification in ER(-) p53-mutated breast cancer patients could significantly improve their response., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2010

6. Cyclophosphamide dose intensification may circumvent anthracycline resistance of p53 mutant breast cancers.

Author

Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Mazouni, Chafika, Giacchetti, S, Turpin, Elisabeth, Espié, Marc, Plassa, Louis-François, Marty, Michel, Bertheau, Philippe, Sotiriou, Christos, Piccart-Gebhart, Martine, Symmans, W Fraser, Pusztai, Lajos, de Thé, Hugues, Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Mazouni, Chafika, Giacchetti, S, Turpin, Elisabeth, Espié, Marc, Plassa, Louis-François, Marty, Michel, Bertheau, Philippe, Sotiriou, Christos, Piccart-Gebhart, Martine, Symmans, W Fraser, Pusztai, Lajos, and de Thé, Hugues

Abstract

The predictive value of p53 for the efficacy of front-line anthracycline-based chemotherapy regimens has been a matter of significant controversy. Anthracyclines are usually combined with widely different doses of alkylating agents, which may significantly modulate tumor response to these combinations. We analyzed three series of de novo stage II-III breast cancer patients treated front line with anthracycline-based regimens of various cyclophosphamide dose intensities: 65 patients with estrogen receptor (ER)(-) tumors treated with anthracyclines alone (Institut Jules Bordet, Brussels), 51 unselected breast cancer patients treated with intermediate doses of cyclophosphamide (MD Anderson Cancer Center, Houston, TX), and 128 others treated with a dose-dense anthracycline-cyclophosphamide combination (St. Louis, Paris). After chemotherapy and surgery, pathologic complete response (pCR) was evaluated. p53 status was determined by a yeast functional assay on the pretreatment tumor sample. In a multivariate analysis of the pooled results, a lack of ER expression and high-dose cyclophosphamide administration were associated with a higher likelihood of pCR. A sharp statistical interaction was detected between p53 status and cyclophosphamide dose intensity. Indeed, when restricting our analysis to patients with ER(-) tumors, we confirmed that a mutant p53 status was associated with anthracycline resistance, but found that p53 inactivation was required for response to the dose-intense alkylating regimen. The latter allowed very high levels of pCR in triple-negative tumors. Thus, our data strongly suggest that cyclophosphamide dose intensification in ER(-) p53-mutated breast cancer patients could significantly improve their response., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2010

7. p53 mutations to predict efficacy of alkylating-containing regimen: a metaanalysis of four different clinical trials

Author

Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Giacchetti, S, Sotiriou, Christos, Turpin, Elisabeth, Espié, Marc, Marty, Marc, Piccart-Gebhart, Martine, Pusztai, Lajos, de Thé, Hugues, Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Giacchetti, S, Sotiriou, Christos, Turpin, Elisabeth, Espié, Marc, Marty, Marc, Piccart-Gebhart, Martine, Pusztai, Lajos, and de Thé, Hugues

Abstract

Asbtract 6064, info:eu-repo/semantics/published

Published

2009

8. p53 mutations to predict efficacy of alkylating-containing regimen: a metaanalysis of four different clinical trials

Author

Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Giacchetti, S, Sotiriou, Christos, Turpin, Elisabeth, Espié, Marc, Marty, Marc, Piccart-Gebhart, Martine, Pusztai, Lajos, de Thé, Hugues, Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Giacchetti, S, Sotiriou, Christos, Turpin, Elisabeth, Espié, Marc, Marty, Marc, Piccart-Gebhart, Martine, Pusztai, Lajos, and de Thé, Hugues

Abstract

Asbtract 6064, info:eu-repo/semantics/published

Published

2009

9. p53 mutations to predict efficacy of alkylating-containing regimen: a metaanalysis of four different clinical trials.

Author

SABCS - San Antonio Breast Cancer Symposium (Jan 15, 2009: San Antonio, Tx, USA), Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Giacchetti, Manuela, Sotiriou, Christos, Turpin, Elisabeth, Espié, Marc, Piccart-Gebhart, Martine, Pusztai, Lajos, de Thé, Hughes, SABCS - San Antonio Breast Cancer Symposium (Jan 15, 2009: San Antonio, Tx, USA), Lehmann-Che, Jacqueline, Andre, Fabrice, Desmedt, Christine, Giacchetti, Manuela, Sotiriou, Christos, Turpin, Elisabeth, Espié, Marc, Piccart-Gebhart, Martine, Pusztai, Lajos, and de Thé, Hughes

Abstract

Poster Session VI: Prognosis and Response Predictions: Response Predictions - Biomarkers and Other Factors; abstract 6064, info:eu-repo/semantics/nonPublished

Published

2009

10. Risques héréditaires de cancers du sein et de l'ovaire : quelle prise en charge ?

Author

Alby, Nicole, Andrieu, Nadine, Auclerc, Gérard, Birnbaum, Daniel, Bonaïti Pellié, Catherine, Brémond, Alain, Bressac de Paillerets, Brigitte, Buy, Jean Noël, Dauplat, Jacques, Demenais, Florence, Eisinger, François, Erriau, Gilles, Espié, Marc, Essioux, Laurent, Feingold, Josué, Ghossain, Michel, Jacquemier, Jocelyne, Janiaud, Paul, Julian Reynier, Claire, Koeger, Anne Claude, Kuttenn, Frédérique, Lefranc, Jean-Pierre, Lehmann, Andrée, Moatti, Jean Paul, Noguès, Catherine, Olschwang, Sylviane, Orsi, Fabienne, Petoin, Sylvain, Pierret, Janine, Pujol, Henri, Regal, Robert, Sasco, Annie J., Serin, Daniel, Schaffer, Paul, Sobol, Hagay, Stoppa, Dominique, Thouvenin, Dominique, Tosi, Mario, Tristant, Henri, Vadrot, Dominique, Institut national de la santé et de la recherche médicale, Alby, Nicole, Andrieu, Nadine, Auclerc, Gérard, Birnbaum, Daniel, Bonaïti Pellié, Catherine, Brémond, Alain, Bressac de Paillerets, Brigitte, Buy, Jean Noël, Dauplat, Jacques, Demenais, Florence, Eisinger, François, Erriau, Gilles, Espié, Marc, Essioux, Laurent, Feingold, Josué, Ghossain, Michel, Jacquemier, Jocelyne, Janiaud, Paul, Julian Reynier, Claire, Koeger, Anne Claude, Kuttenn, Frédérique, Lefranc, Jean-Pierre, Lehmann, Andrée, Moatti, Jean Paul, Noguès, Catherine, Olschwang, Sylviane, Orsi, Fabienne, Petoin, Sylvain, Pierret, Janine, Pujol, Henri, Regal, Robert, Sasco, Annie J., Serin, Daniel, Schaffer, Paul, Sobol, Hagay, Stoppa, Dominique, Thouvenin, Dominique, Tosi, Mario, Tristant, Henri, Vadrot, Dominique, and Institut national de la santé et de la recherche médicale

Abstract

Les recommandations présentées s'appuient sur le travail réalisé pendant 18 mois par un groupe d'experts réunis par l'INSERM à la demande de la Fédération nationale des centres de lutte contre le cancer (FNCLCC). Le groupe a travaillé selon la méthodologie de l'Expertise Collective INSERM, à partir d'une documentation internationale large relative à la génétique des cancers du sein et de l'ovaire, leur prise en charge et les modalités d'organisation de cette dernière. L’ensemble des experts et les commanditaires de l'expertise ont d'emblée été conscients de la difficulté à obtenir un consensus portant sur tous les aspects de la prise en charge dès lors que l'on a affaire à une pratique médicale qui n'est pas encore évaluée. En effet, il s'agit d'un domaine encore trop neuf pour que des standards aient pu d'ores et déjà être établis. Toutefois, le travail de réflexion et d'analyse des références disponibles et la rédaction de recommandations sont apparus comme nécessaires dans le but d'éviter des pratiques médicales non homogènes, mal évaluées et sans références communes. Ce texte est destiné essentiellement à la communauté médicale amenée à prendre en charge les personnes ayant un risque accru, d'origine génétique, de développer un cancer du sein ou de l'ovaire. De ce fait même, le présent document prend avant tout en considération les données médicales mais entend attirer l'attention des médecins sur le fait que cette pratique qui n'est pas encore bien définie se heurte à un certain nombre d'incertitudes et de difficultés. Celles-ci concernent tout d'abord les femmes venues consulter un oncogénéticien: si l'information pour celles d'entre elles qui ne sont pas porteuses de l'anomalie génétique incriminée peut être rassurante, tel n'est pas le cas pour celles qui ont hérité de l'anomalie. Pour ces dernières se pose la question des possibilités qui leur sont offertes de la prise en charge non pas d'une maladie avérée, mais d'un risque de la développer. En outre, la c, 522 pages, figures

Published

2008