TY - JOUR
T1 - Cytogenetic features of de novo CD5-positive diffuse large B-cell lymphoma
T2 - Chromosome aberrations affecting 8p21 and 11q13 constitute major subgroups with different overall survival
AU - Yoshioka, Tomoko
AU - Miura, Ikuo
AU - Kume, Masaaki
AU - Takahashi, Naoto
AU - Okamoto, Masataka
AU - Ichinohasama, Ryo
AU - Yoshino, Tadashi
AU - Yamaguchi, Motoko
AU - Hirokawa, Makoto
AU - Sawada, Ken Ichi
AU - Nakamura, Shigeo
PY - 2005/2
Y1 - 2005/2
N2 - De novo CD5-positive diffuse large B-cell lymphoma (CD5+DLBCL) is regarded as a different clinicopathological entity from CD5-negative DLBCL (CD5-DLBCL) and mantle cell lymphoma (MCL). Because only a few published cytogenetic studies of de novo CD5+DLBCL are available, we investigated chromosomal changes in 23 Japanese patients who had de novo CD5+DLBCL. A characteristic of cytogenetic abnormalities in de novo CD5+DLBCL was a high incidence of chromosomal aberrations affecting 8p21 and 11q13. Major chromosomal breakpoints were concentrated at 8p21, 11q13, and 3q27. Patients with 8p21 aberrations showed aggressive clinical features, including advanced stage of disease, elevated serum LDH level, poor performance status, and an inferior survival curve compared with patients who had 11q13 changes (P = .043). Chromosomal abnormalities of both 8p21 and 11q13 were not observed in the same patient, and each abnormality showed different chromosomal gains and losses. These results indicate that de novo CD5+DLBCL may occur in previously unidentified subgroups that differ in their chromosomal abnormalities. The conflicting results of previous studies on prognosis may thus be explained in part by the differences in chromosomal changes.
AB - De novo CD5-positive diffuse large B-cell lymphoma (CD5+DLBCL) is regarded as a different clinicopathological entity from CD5-negative DLBCL (CD5-DLBCL) and mantle cell lymphoma (MCL). Because only a few published cytogenetic studies of de novo CD5+DLBCL are available, we investigated chromosomal changes in 23 Japanese patients who had de novo CD5+DLBCL. A characteristic of cytogenetic abnormalities in de novo CD5+DLBCL was a high incidence of chromosomal aberrations affecting 8p21 and 11q13. Major chromosomal breakpoints were concentrated at 8p21, 11q13, and 3q27. Patients with 8p21 aberrations showed aggressive clinical features, including advanced stage of disease, elevated serum LDH level, poor performance status, and an inferior survival curve compared with patients who had 11q13 changes (P = .043). Chromosomal abnormalities of both 8p21 and 11q13 were not observed in the same patient, and each abnormality showed different chromosomal gains and losses. These results indicate that de novo CD5+DLBCL may occur in previously unidentified subgroups that differ in their chromosomal abnormalities. The conflicting results of previous studies on prognosis may thus be explained in part by the differences in chromosomal changes.
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U2 - 10.1002/gcc.20127
DO - 10.1002/gcc.20127
M3 - Article
C2 - 15543600
AN - SCOPUS:19944426055
SN - 1045-2257
VL - 42
SP - 149
EP - 157
JO - Genes Chromosomes and Cancer
JF - Genes Chromosomes and Cancer
IS - 2
ER -