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Bcl2 Over-Expression as a Prognostic factor In Hodgkin Lymphoma Patients who Required Intensive Treatment

Authors :
Jorge Gayoso
Pascual Balsalobre
Cristina Muñoz-Martínez
Isabel Gonzalez
Javier Menárguez
Mi Kwon
Antonio Escudero
Patricia Font
José Luis Díez-Martín
Santiago Osorio
Leyre Bento
Cristina Encinas
Gabriela Rodríguez-Macías
David P. Serrano
Source :
Blood. 116:4825-4825
Publication Year :
2010
Publisher :
American Society of Hematology, 2010.

Abstract

Abstract 4825 Introduction: The majority of patients with classical Hodgkinxs Lymphoma (cHL) are cured with primary treatment. However, a significant proportion of patients will not achieve a complete response (CR) or relapse after completion of initial therapy and need to be rescued with high-dose chemotherapy and stem cell transplantation (SCT): autologous (aSCT) and/or alogeneic (Alo-SCT). The identification of clinical and biological characteristics of these patients at diagnosis is still a challenge and the most prognostic systems used to date fail to identify a proportion of patients with worse prognosis. The best understanding of the biology of cHL could help to identify these patients and different groups works in the use of biological marker as determinants of clinical outcome. Bcl2 over-expression has been described in cHL and seems to be an independent marker associated to bad prognosis in probably relation with alterations in apoptosis regulatory molecules. Objetive: To retrospectively analyze the frequency of Bcl2 protein over-expression in tissue biopsies of patients diagnosed with cHL, which required intensive treatment in our centre. Patients and Methods: We revised clinical data and samples at diagnosis of patients with cHL who received SCT (aSCT or/and Allo-SCT) due to partial remission, relapse or progression and we determined Bcl2 expression protein by immunohistochemistry. All patients received at least 2 lines of treatment previous to intensive treatment with SCT. We analyzed the expression of Bcl2 according to each patient histology: Nodular Sclerosis (NE), Mixed cellularity (MC), Lymphocyte-rich (LR), and Lymphocyte-depleted (LD). Results: Between September 1997 and May 2010, 39 patients with cHL required intensive treatment in our center: 32 aSCT and 7 Allo-SCT due to partial remission, refractory, relapse or progression after first line of treatment. Average age was 32 years (range: 18–64), males: 25/females 14. The characteristics of patients and remission status at transplant are described in table 1. We had available samples at diagnosis from 31 out of 39 patients (80%): 20 NE, 5 MC, 6 LR and we found over-expression of Bcl2 in 17/20 (85%) NE; 5/5(100%) MC and 2/6 LR (33%). Conclusions: Our results suggest that over-expression of Bcl2 is frequent in patients with cHL which needed intensive treatment after failure of the first line of therapy (particularly with NE and MC). Further studies are needed to confirm the worse prognosis of Bcl2 expression in cHL and if may be useful at diagnosis in association with other clinical parameters to identify patients with poor prognosis. Table 1 . CLASSICAL HODGKIN LYMPHOMA (c HL) NODULAR SCLEROSIS cHL MIXED CELLULARITY cHL LYMPHOCYTE-RICH cHL LYMPHOCYTE-DEPLETED cHL N (39) 23 8 7 1 Sex (F/M) 11/12 8/0 5/2 1/0 Age, Years: Md(R) 30(18-64) 37(31-62) 36(19-64) 54 Stage: I, II/III, IV 11/12 3/5 5/2 0/1 Bulky disease 14YES/9NO 1YES/7NO 2YES/5NO 1NO B Symptoms: (N) YES/NO (13) YES/(10) NO (3) YES/(5) NO (6) YES/(1) NO (1) YES Intensive treatment 5Alo-SCT/18aSCT 2AloSCT/6aSCT 7aSCT 1aSCT N:type of trasplant (status at transplant) 18: aSCT(11CR/5PR/2RF); 5:AloSCT(2PR with previous aSCT/1PR/1CR/1RF) 6: aSCT (4CR/2PR) 7:aSCT (6CR/1PR) 1:aSCT (in CR) 2: Alo-SCT(1CR/1PR with previus aSCT) Sample revised: N 20 (23 total NE) 5 (8 total MC) 6 (7 total LR) 0/1 Bcl2 expression: P/Nv (%) 17P/3Nv (85%) 5P/0Nv (100%) 2P/4Nv (33%) Not aplicable Alo-SCT: Alogeneic stem cell transplant; aSCT: autologous stem cell transplant; CR: Complete Remission; F: female; LD: Lymphocyte-deplete; LR: Lymphocyte rich; M: male; MC: mixed cellularity Md: median; n: number; NE: nodular sclerosis; Nv: negative; P: positive; PR: Parcial remision R: range; RF: refractory Disclosures: No relevant conflicts of interest to declare.

Details

ISSN :
15280020 and 00064971
Volume :
116
Database :
OpenAIRE
Journal :
Blood
Accession number :
edsair.doi...........41a4a232cc3cc655c8a77d6f7b4116a7