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Blood.
2006 Oct 1;108(7):2373-83. Epub 2006 Jun 13.
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High BCL6 expression predicts better prognosis,
independent of BCL6 translocation status,
translocation partner, or BCL6-deregulating
mutations, in gastric lymphoma.
Chen
YW,
Hu XT, Liang AC, Au WY, So CC, Wong ML, Shen L, Tao
Q, Chu KM, Kwong YL, Liang RH, Srivastava G.
Department of Pathology, Li Ka Shing Faculty of
Medicine, The University of Hong Kong, Hong Kong.
To investigate the role of BCL6
in the pathogenesis of gastric lymphoma, we analyzed
the BCL6 promoter region for BCL6 translocations,
somatic hypermutations, and deregulating mutations
in 43 gastric lymphomas, including 4 extranodal
marginal-zone B-cell lymphomas of mucosa-associated
lymphoid tissues (MALT lymphomas), 33 diffuse large
B-cell lymphomas (DLBCLs), and 6 composite DLBCLs
with residual MALT lymphoma (DLCLMLs). BCL6 promoter
substitutions by immunoglobulin (Ig) and non-Ig
translocation partners, resulting in its
deregulation, were frequently involved in DLBCL
(36.4%) and DLCLML (50%). Two novel BCL6
translocation partner genes, 28S rRNA and DMRT1, and
a new BCL6 translocation breakpoint in intron 2 were
also identified. Deregulating mutations were found
only in DLBCL (24.2%), which correlated
significantly with high BCL6 protein expression.
Significantly, high BCL6 expression correlated
strongly with longer overall survival (OS),
independent of mechanism in gastric DLBCL and DLCLML.
Gastric DLBCLs were further subclassified into
germinal center B-cell-like (GCB) and non-GCB
subgroups immunohistochemically. High BCL6
expression was detected in all GCB cases,
irrespective of BCL6 genetic alterations. In the
non-GCB subgroup, BCL6-deregulating mutations
correlated significantly with high BCL6 expression
level. No significant correlation was found between
the BCL6 expression level and OS in the non-GCB
subgroup, which had significantly poorer prognosis
than the GCB subgroup.
PMID: 16772602 [PubMed - indexed for
MEDLINE]