Your search keyword '"Soubeyran, I."' showing total 6 results

1. IGHV gene features and MYD88 L265P mutation separate the three marginal zone lymphoma entities and Waldenström macroglobulinemia/lymphoplasmacytic lymphomas.

Author

Gachard, N, Parrens, M, Soubeyran, I, Petit, B, Marfak, A, Rizzo, D, Devesa, M, Delage-Corre, M, Coste, V, Laforêt, M P, de Mascarel, A, Merlio, J P, Bouabdhalla, K, Milpied, N, Soubeyran, P, Schmitt, A, Bordessoule, D, Cogné, M, and Feuillard, J

Subjects

LYMPHOMAS, IMMUNOGLOBULINS, SPLEEN, LYMPH nodes, MUCOUS membranes

Abstract

To clarify the relationships between marginal zone lymphomas (MZLs) and Waldenström macroglobulinemia/lymphoplasmacytic lymphomas (WM/LPLs), immunoglobulin heavy chain variable gene (IGHV) features were analyzed and the occurrence of MYD88 L265P mutations was identified in a series of 123 patients: 53 MZLs from the spleen (SMZLs), 11 from lymph nodes (NMZLs), 28 mucosa-associated lymphatic tissue (MALT) lymphomas and 31 WM/LPLs. SMZLs were characterized by overrepresentation of IGHV1-2 gene rearrangements with a canonical motif, without selection pressure and with long CDR3 segments. NMZLs had increased frequencies of IGHV3 genes. The IGHV gene was unmutated in most cases, often with long CDR3 segments. MALT lymphomas were usually associated with a mutated IGHV gene, but with the absence of selection pressure. WM/LPLs were associated with an IGHV3-23 overrepresentation and high IGHV mutation rate, with features of selection pressure and short CDR3 segments. MYD88 L265P mutations were almost restricted exclusively to WM/LPL patients. Taken all diagnoses together, all patients with MYD88 L265P mutations had an immunoglobulin M peak and almost all patients except one had bone marrow infiltration. These results demonstrate that the history of antigen exposure of the four entities studied was different and MYD88 L265P was specifically associated with WM/LPLs. WM/LPL may thus be functionally associated with constitutive nuclear factor-κB activation. [ABSTRACT FROM AUTHOR]

Published

2013

2. Splenic marginal zone lymphomas and lymphoplasmacytic lymphomas originate from B-cell compartments with two different antigen-exposure histories.

Author

Parrens, M., Garchard, N., Petit, B., Marfak, A., Troadec, E., Bouabdhalla, K., Milpied, N., Merlio, J. P., de Mascarel, A., Laurent, C., Soubeyran, I., Coste, V., Labrousse, F., Cogné, M., and Feuillard, J.

Subjects

LETTERS to the editor, LYMPHOMAS

Abstract

A letter to the editor is presented which discusses the origin of splenic marginal zone lymphomas and lymphoplasmacytic lymphomas from B-cell compartments with two different antigen-exposure histories.

Published

2008

3. Evolution of BCL-2/IgH hybrid gene RNA expression during treatment of T(14;18)-bearing follicular lymphomas.

Author

Soubeyran, P, Hostein, I, Debled, M, Eghbali, H, Soubeyran, I, Bonichon, F, Astier-Gin, T, and Hœrni, B

Subjects

LYMPHOMAS, DRUG therapy

Abstract

Bcl-2, the gene over-expressed in follicular lymphomas (FL), is able to block chemotherapy-induced apoptosis. Consequently, we wondered whether bcl-2/IgH expression variations during treatment of FL could predict the outcome of patients with t(14;18)-bearing FL. For this purpose, we used a reverse transcription polymerase chain reaction (RT-PCR) assay to analyse 180 serial peripheral blood samples (PBS) during 34 treatment phases in 25 patients with t(14;18)-bearing FL. In all patients but two, bcl-2/IgH gene expression was demonstrated in pre-treatment samples. During 16 out of the 34 treatment phases (47%), bcl-2/IgH expression became negative: all but one were responders to chemotherapy. This conversion was transient in six cases. In 18 treatment phases, bcl2/IgH expression remained detectable: eight were clinically considered as treatment failures, while eight others achieved PR and two achieved CR. We observed a significant correlation between treatment response and RNA PCR results (P = 0.002). Three-year overall survival of patients with stable bcl2/IgH-negative conversion was 100% compared to 54% for the remaining patients (P = 0.069); 3-year freedom from progression was respectively 87.5% and 13% (P = 0.005). These results indicate a correlation between bcl-2/IgH expression variations and both clinical response and outcome. Whether this might predict disease outcome early remains to be confirmed. [ABSTRACT FROM AUTHOR]

Published

1999

4. pS2 protein: a marker improving prediction of response to neoadjuvant tamoxifen in post-menopausal breast cancer patients.

Author

Soubeyran, I, Quénel, N, Coindre, J-M, Bonichon, F, Durand, M, Wafflart, J, Mauriac, L, and Quénel, N

Published

1996

5. Variation of hormonal receptor, pS2, c-erbB-2 and GSTpi contents in breast carcinomas under tamoxifen: a study of 74 cases.

Author

Soubeyran, I, Quénel, N, Mauriac, L, Durand, M, Bonichon, F, Coindre, J-M, Quénel, N, and Coindre J-M

Published

1996

6. Tumor fraction-based prognostic tool for cancer patients referred to early phase clinical trials.

Author

Bayle A, Belcaid L, Cousin S, Trin K, Alame M, Rouleau E, Soubeyran I, Lacroix L, Blouin L, Vasseur D, Crombe A, Mathoulin-Pelissier S, Soria JC, Bellera C, and Italiano A

Abstract

Selecting patients for phase I cancer trials is crucial to ensure a sufficient life expectancy. Frail patients, better suited for palliative care, should not be exposed to new drugs with minimal benefit. Enrolling patients at high risk of early death can jeopardize the study. Our analysis of two large precision medicine studies used tumor fraction from ctDNA to develop a predictive model, demonstrating notable predictive accuracy and aiding in patient selection., (© 2024. The Author(s).)

Published

2024