Your search keyword '"Rothé, Françoise"' showing total 6 results

1. Unraveling Triple-Negative Breast Cancer Tumor Microenvironment Heterogeneity: Towards an Optimized Treatment Approach

Author

Bareche, Yacine, primary, Buisseret, Laurence, additional, Gruosso, Tina, additional, Girard, Edwina, additional, Venet, David, additional, Dupont, Floriane, additional, Desmedt, Christine, additional, Larsimont, Denis, additional, Park, Morag, additional, Rothé, Françoise, additional, Stagg, John, additional, and Sotiriou, Christos, additional

Published

2019

2. Unraveling Triple-Negative Breast Cancer Tumor Microenvironment Heterogeneity: Towards an Optimized Treatment Approach.

Author

Bareche, Yacine, Buisseret, Laurence, Gruosso, Tina, Girard, Edwina, Venet, David, Dupont, Floriane, Desmedt, Christine, Larsimont, Denis, Park, Morag, Rothé, Françoise, Stagg, John, and Sotiriou, Christos

Subjects

TRIPLE-negative breast cancer, BREAST tumors, TUMOR microenvironment, ANDROGEN receptors, GENE expression profiling

Abstract

Background: Recent efforts of gene expression profiling analyses recognized at least four different triple-negative breast cancer (TNBC) molecular subtypes. However, little is known regarding their tumor microenvironment (TME) heterogeneity.Methods: Here, we investigated TME heterogeneity within each TNBC molecular subtype, including immune infiltrate localization and composition together with expression of targetable immune pathways, using publicly available transcriptomic and genomic datasets from a large TNBC series totaling 1512 samples. Associations between molecular subtypes and specific features were assessed using logistic regression models. All statistical tests were two-sided.Results: We demonstrated that each TNBC molecular subtype exhibits distinct TME profiles associated with specific immune, vascularization, stroma, and metabolism biological processes together with specific immune composition and localization. The immunomodulatory subtype was associated with the highest expression of adaptive immune-related gene signatures and a fully inflamed spatial pattern appearing to be the optimal candidate for immune check point inhibitors. In contrast, most mesenchymal stem-like and luminal androgen receptor tumors showed an immunosuppressive phenotype as witnessed by high expression levels of stromal signatures. Basal-like, luminal androgen receptor, and mesenchymal subtypes exhibited an immune cold phenotype associated with stromal and metabolism TME signatures and enriched in margin-restricted spatial pattern. Tumors with high chromosomal instability and copy number loss in the chromosome 5q and 15q regions, including genomic loss of major histocompatibility complex related genes, showed reduced cytotoxic activity as a plausible immune escape mechanism.Conclusions: Our results demonstrate that each TNBC subtype is associated with specific TME profiles, setting the ground for a rationale tailoring of immunotherapy in TNBC patients. [ABSTRACT FROM AUTHOR]

Published

2020

3. Tumor-Infiltrating Lymphocytes in Patients Receiving Trastuzumab/Pertuzumab-Based Chemotherapy: A TRYPHAENA Substudy

Author

Ignatiadis, Michail, primary, Van den Eynden, Gert, additional, Roberto, Salgado, additional, Fornili, Marco, additional, Bareche, Yacine, additional, Desmedt, Christine, additional, Rothé, Françoise, additional, Maetens, Marion, additional, Venet, David, additional, Holgado, Esther, additional, McNally, Virginia, additional, Kiermaier, Astrid, additional, Savage, Heidi M, additional, Wilson, Timothy R, additional, Cortes, Javier, additional, Schneeweiss, Andreas, additional, Willard-Gallo, Karen, additional, Biganzoli, Elia, additional, and Sotiriou, Christos, additional

Published

2018

4. Circulating Tumor Cells in Breast Cancer Patients Treated by Neoadjuvant Chemotherapy: A Meta-analysis

Author

Bidard, François-Clément, primary, Michiels, Stefan, additional, Riethdorf, Sabine, additional, Mueller, Volkmar, additional, Esserman, Laura J, additional, Lucci, Anthony, additional, Naume, Bjørn, additional, Horiguchi, Jun, additional, Gisbert-Criado, Rafael, additional, Sleijfer, Stefan, additional, Toi, Masakazu, additional, Garcia-Saenz, Jose A, additional, Hartkopf, Andreas, additional, Generali, Daniele, additional, Rothé, Françoise, additional, Smerage, Jeffrey, additional, Muinelo-Romay, Laura, additional, Stebbing, Justin, additional, Viens, Patrice, additional, Magbanua, Mark Jesus M, additional, Hall, Carolyn S, additional, Engebraaten, Olav, additional, Takata, Daisuke, additional, Vidal-Martínez, José, additional, Onstenk, Wendy, additional, Fujisawa, Noriyoshi, additional, Diaz-Rubio, Eduardo, additional, Taran, Florin-Andrei, additional, Cappelletti, Maria Rosa, additional, Ignatiadis, Michail, additional, Proudhon, Charlotte, additional, Wolf, Denise M, additional, Bauldry, Jessica B, additional, Borgen, Elin, additional, Nagaoka, Rin, additional, Carañana, Vicente, additional, Kraan, Jaco, additional, Maestro, Marisa, additional, Brucker, Sara Yvonne, additional, Weber, Karsten, additional, Reyal, Fabien, additional, Amara, Dominic, additional, Karhade, Mandar G, additional, Mathiesen, Randi R, additional, Tokiniwa, Hideaki, additional, Llombart-Cussac, Antonio, additional, Meddis, Alessandra, additional, Blanche, Paul, additional, d'Hollander, Koenraad, additional, Cottu, Paul, additional, Park, John W, additional, Loibl, Sibylle, additional, Latouche, Aurélien, additional, Pierga, Jean-Yves, additional, and Pantel, Klaus, additional

Published

2018

5. Immune Infiltration in Invasive Lobular Breast Cancer

Author

Desmedt, Christine, primary, Salgado, Roberto, additional, Fornili, Marco, additional, Pruneri, Giancarlo, additional, Van den Eynden, Gert, additional, Zoppoli, Gabriele, additional, Rothé, Françoise, additional, Buisseret, Laurence, additional, Garaud, Soizic, additional, Willard-Gallo, Karen, additional, Brown, David, additional, Bareche, Yacine, additional, Rouas, Ghizlane, additional, Galant, Christine, additional, Bertucci, François, additional, Loi, Sherene, additional, Viale, Giuseppe, additional, Di Leo, Angelo, additional, Green, Andrew R, additional, Ellis, Ian O, additional, Rakha, Emad A, additional, Larsimont, Denis, additional, Biganzoli, Elia, additional, and Sotiriou, Christos, additional

Published

2018

6. Tumor-Infiltrating Lymphocytes in Patients Receiving Trastuzumab/Pertuzumab-Based Chemotherapy: A TRYPHAENA Substudy.

Author

Ignatiadis, Michail, Eynden, Gert Van den, Roberto, Salgado, Fornili, Marco, Bareche, Yacine, Desmedt, Christine, Rothé, Françoise, Maetens, Marion, Venet, David, Holgado, Esther, McNally, Virginia, Kiermaier, Astrid, Savage, Heidi M, Wilson, Timothy R, Cortes, Javier, Schneeweiss, Andreas, Willard-Gallo, Karen, Biganzoli, Elia, Sotiriou, Christos, and Van den Eynden, Gert

Subjects

LYMPHOCYTES, TRASTUZUMAB, CANCER chemotherapy, EPIDERMAL growth factor, PATHOLOGY

Abstract

Background: There is an urgent requirement to identify biomarkers to tailor treatment in human epidermal growth factor receptor 2 (HER2)-amplified early breast cancer treated with trastuzumab/pertuzumab-based chemotherapy.Methods: Among the 225 patients randomly assigned to trastuzumab/pertuzumab concurrently or sequentially with an anthracycline-containing regimen or concurrently with an anthracycline-free regimen in the Tryphaena trial, we determined the percentage of tumor-infiltrating lymphocytes (TILs) at baseline in 213 patients, of which 126 demonstrated a pathological complete response (pCR; ypT0/is ypN0), with 28 demonstrating event-free survival (EFS) events. We investigated associations between baseline TIL percentage and either pCR or EFS after adjusting for clinicopathological characteristics using logistic and Cox regression models, respectively. To understand TIL biology, we evaluated associations between baseline TILs and baseline tumor gene expression data (800 gene set by NanoString) in a subset of 173 patients. All statistical tests were two-sided.Results: Among the patients with measurable TILs at baseline, the median level was 14.1% (interquartile range = 7.1%-32.4%). After adjusting for clinicopathological characteristics, baseline percentage TIL was not associated with pCR (adjusted odds ratio [aOR] for every 10-percentage unit increase in TILs = 1.12, 95% confidence interval [CI] = 0.95 to 1.31, P = .17). At a median follow-up of 4.7 years, for every increase in baseline TILs of 10%, there was a 25% reduction in the hazard for an EFS event (aOR = 0.75, 95% CI = 0.56 to 1.00, P = .05) after adjusting for baseline clinicopathological characteristics and pCR. Additionally, genes associated with epithelial-mesenchymal transition, angiogenesis, and T-cell inhibition such as SNAIL1, ZEB1, NOTCH3, and B7-H3 were statistically significantly inversely correlated with percentage TIL.Conclusions: Baseline TIL percentage provides independent prognostic information in patients treated with trastuzumab/pertuzumab-based neoadjuvant chemotherapy. However, further validation is required. [ABSTRACT FROM AUTHOR]

Published

2019