TY - JOUR
T1 - Proliferation centers in chronic lymphocytic leukemia
T2 - Correlation with cytogenetic and clinicobiological features in consecutive patients analyzed on tissue microarrays
AU - Ciccone, M.
AU - Agostinelli, C.
AU - Rigolin, G. M.
AU - Piccaluga, P. P.
AU - Cavazzini, F.
AU - Righi, S.
AU - Sista, M. T.
AU - Sofritti, O.
AU - Rizzotto, L.
AU - Sabattini, E.
AU - Fioritoni, G.
AU - Falorio, S.
AU - Stelitano, C.
AU - Olivieri, A.
AU - Attolico, I.
AU - Brugiatelli, M.
AU - Zinzani, P. L.
AU - Saccenti, E.
AU - Capello, D.
AU - Negrini, M.
AU - Cuneo, A.
AU - Pileri, S.
N1 - Funding Information:
This work was supported by funding from AIL-FE, AIRC regional grants, MIUR (PRIN), by Emilia Romagna regional grants to AC and by grants from: 1) the Associazione Italiana Ricerca contro il Cancro (AIRC, Milan, Italy), including the Special Program Molecular Clinical Oncology, 5%, No. 10007 (SAP) and 2) Interdepartmental Centre for Cancer Research ‘Giorgio Prodi’ (Bologna, Italy). LR is supported by AIL-FE. We thank the following clinicians who provided follow-up data: Giampiero Bellesi (Firenze), Bruno Benci (Arezzo), Cinzia Bonanno (Palermo), Nicola Cantore (Benevento), Stefania Ciolli (Firenze), Alfonso Maria D’Arco (Nocera Inferiore), Maurizio Martelli (Roma), Roberto Ranalli (Sulmona), Alfonso Zaccaria (Ravenna), Francesco Zaja (Udine), Alberto Grossi (Firenze), Alberto Fragasso (Matera), Vallone Roberto (BN), Fortunato Morabito (Cosenza), Guglielo Mariani (AQ), Roberto Ranalli (Sulmona) and Paolo Vivaldi (TN).
PY - 2012/3
Y1 - 2012/3
N2 - To better define the significance of proliferation centers (PCs), the morphological hallmark of chronic lymphocytic leukemia (CLL), lymph node biopsies taken from 183 patients were submitted to histopathologic and fluorescence in situ hybridization (FISH) studies using a 5-probe panel on tissue microarrays. Seventy-five cases (40.9%) with confluent PCs were classified as 'PCs-rich' and 108 cases (59.1%) with scattered PCs were classified as 'typical'. Complete FISH data were obtained in 101 cases (55.1%), 79 of which (78.2%) displayed at least one chromosomal aberration. The incidence of each aberration was: 13q- 36,7%, 14q32 translocations 30.8%, 11q- 24.7%, trisomy 12 19.5% and 17p- 15.6%. Five cases showed extra copies of the 14q32 region. The 'PCs-rich' group was associated with 17p-, 14q32/IgH translocation, +12, Ki-67>30%. The median survival from the time of tissue biopsy for PCs-rich and typical groups was 11 and 64 months, respectively (P=0.00001). The PCs-rich pattern was the only predictive factor of an inferior survival at multivariate analysis (P=0.022). These findings establish an association between cytogenetic profile and the amount of PC in CLL, and show that this histopathologic characteristic is of value for risk assessment in patients with clinically significant adenopathy.
AB - To better define the significance of proliferation centers (PCs), the morphological hallmark of chronic lymphocytic leukemia (CLL), lymph node biopsies taken from 183 patients were submitted to histopathologic and fluorescence in situ hybridization (FISH) studies using a 5-probe panel on tissue microarrays. Seventy-five cases (40.9%) with confluent PCs were classified as 'PCs-rich' and 108 cases (59.1%) with scattered PCs were classified as 'typical'. Complete FISH data were obtained in 101 cases (55.1%), 79 of which (78.2%) displayed at least one chromosomal aberration. The incidence of each aberration was: 13q- 36,7%, 14q32 translocations 30.8%, 11q- 24.7%, trisomy 12 19.5% and 17p- 15.6%. Five cases showed extra copies of the 14q32 region. The 'PCs-rich' group was associated with 17p-, 14q32/IgH translocation, +12, Ki-67>30%. The median survival from the time of tissue biopsy for PCs-rich and typical groups was 11 and 64 months, respectively (P=0.00001). The PCs-rich pattern was the only predictive factor of an inferior survival at multivariate analysis (P=0.022). These findings establish an association between cytogenetic profile and the amount of PC in CLL, and show that this histopathologic characteristic is of value for risk assessment in patients with clinically significant adenopathy.
KW - 14q32 translocation
KW - FISH
KW - chronic lymphocytic leukemia
KW - proliferation centers
KW - small lymphocytic lymphoma
UR - http://www.scopus.com/inward/record.url?scp=84858001439&partnerID=8YFLogxK
U2 - 10.1038/leu.2011.247
DO - 10.1038/leu.2011.247
M3 - Article
SN - 0887-6924
VL - 26
SP - 499
EP - 508
JO - Leukemia
JF - Leukemia
IS - 3
ER -