Your search keyword '"Schmitt, Yohann"' showing total 2 results

1. Diffuse gliomas with FGFR3‐TACC3 fusion have characteristic histopathological and molecular features.

Author

Bielle, Franck, Di Stefano, Anna‐Luisa, Meyronet, David, Picca, Alberto, Villa, Chiara, Bernier, Michèle, Schmitt, Yohann, Giry, Marine, Rousseau, Audrey, Figarella‐Branger, Dominique, Maurage, Claude‐Alain, Uro‐Coste, Emmanuelle, Lasorella, Anna, Iavarone, Antonio, Sanson, Marc, and Mokhtari, Karima

Subjects

GLIOMAS, CHEMORADIOTHERAPY, HISTOPATHOLOGY, FIBROBLAST growth factor receptors, DIFFUSE large B-cell lymphomas

Abstract

Adult glioblastomas, IDH‐wildtype represent a heterogeneous group of diseases. They are resistant to conventional treatment by concomitant radiochemotherapy and carry a dismal prognosis. The discovery of oncogenic gene fusions in these tumors has led to prospective targeted treatments, but identification of these rare alterations in practice is challenging. Here, we report a series of 30 adult diffuse gliomas with an in frame FGFR3‐TACC3 oncogenic fusion (n = 27 WHO grade IV and n = 3 WHO grade II) as well as their histological and molecular features. We observed recurrent morphological features (monomorphous ovoid nuclei, nuclear palisading and thin parallel cytoplasmic processes, endocrinoid network of thin capillaries) associated with frequent microcalcifications and desmoplasia. We report a constant immunoreactivity for FGFR3, which is a valuable method for screening for the FGFR3‐TACC3 fusion with 100% sensitivity and 92% specificity. We confirmed the associated molecular features (typical genetic alterations of glioblastoma, except the absence of EGFR amplification, and an increased frequency of CDK4 and MDM2 amplifications). FGFR3 immunopositivity is a valuable tool to identify gliomas that are likely to harbor the FGFR3‐TACC3 fusion for inclusion in targeted therapeutic trials. [ABSTRACT FROM AUTHOR]

Published

2018

2. Chromosome 17p Homodisomy Is Associated With Better Outcome in 1p19q Non-Codeleted and IDH-Mutated Gliomas.

Author

Labussière, Marianne, Rahimian, Amithys, Giry, Marine, Boisselier, Blandine, Schmitt, Yohann, Polivka, Marc, Mokhtari, Karima, Delattre, Jean‐Yves, Idbaih, Ahmed, Labreche, Karim, Alentorn, Agusti, and Sanson, Marc

Subjects

CHI-squared test, GLIOMAS, CHROMOSOMES, DNA, FISHER exact test, GENES, GENETIC polymorphisms, GENOMES, LONGITUDINAL method, GENETIC mutation, PROPORTIONAL hazards models, DISEASE progression, GENETIC carriers, KAPLAN-Meier estimator, SEQUENCE analysis, LOG-rank test, MANN Whitney U Test, PROGNOSIS, GENETICS

Abstract

Background. The 1p19q non-codeleted gliomas with IDH mutation, defined as "molecular astrocytomas," display frequent TP53 mutations and have an intermediate prognosis. We investigated the prognostic impact of copy number-neutral loss of heterozygosity (CNLOH) in 17p in this population. Methods. We analyzed 793 gliomas (206 grade II, 377 grade III, and 210 grade IV) by single nucleotide polymorphism array and for TP53 mutations. Results. Homodisomy revealed by CNLOH was observed in 156 cases (19.7%). It was more frequent in astrocytomas and oligoastrocytomas (98/256, 38%) than oligodendrogliomas (28/327, 8.6%; p < .0001) orglioblastoma multiforme (30/210, 14.3%; p < .0001), tightly associated with TP53 mutation (69/71 vs. 20/79; p = 2 x 10-16), and mutually exclusive with 1p19q codeletion (1/156 vs. 249/556;p < .0001). In the group of IDH-mutated 1p19q non-codeleted gliomas, CNLOH 17p was associated with longer survival (86.3 vs. 46.2 months; p = .004), particularly in grade III gliomas (overall survival .100 vs. 37.9 months; p = .007). These data were confirmed in an independent dataset from the Cancer Genome Atlas. Conclusion. CNLOH 17p is a prognostic marker and further refines the molecular classification of gliomas. [ABSTRACT FROM AUTHOR]

Published

2016